As
filed with the Securities and Exchange Commission on April 20,
2006.
Registration
No. 333-[________]
SECURITIES
AND EXCHANGE COMMISSION
Washington,
D.C. 20549
FORM
F-1
REGISTRATION
STATEMENT
UNDER
THE
SECURITIES ACT OF 1933
XTL BIOPHARMACEUTICALS LTD.
(Exact
Name of Registrant as Specified in its Charter)
|
Israel
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2834
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Not
Applicable
|
|
(State
or Other Jurisdiction of
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(Primary
Standard Industrial
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(I.R.S.
Employer
|
|
Incorporation
or Organization)
|
Classification
Code Number)
|
Identification
Number)
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750 Lexington Avenue, 20th Floor
New
York, NY 10022
(212)
531-5960
(Address,
including zip code, and telephone number, including
area
code, of registrant’s principal executive offices)
Ron Bentsur
Chief
Executive Officer
750
Lexington Avenue, 20th Floor
New
York, NY 10022 (212) 531-5960
(Name,
address, including zip code, and telephone number,
including
area code, of agent for service)
Copies of Communications to:
|
Mark
F. McElreath
|
Ronen
Kantor
|
|
Alston
& Bird LLP
|
Kantor
& Co.
|
|
90
Park Avenue
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Oz
House
|
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New
York, New York 10016
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14
Abba Hilel Silver (12th
Floor)
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(212)
210-9400
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Ramat
Gan 52506, Israel
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(011)
+ 972 3 613 3371
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Approximate
date of commencement of proposed sale to the public:
As soon
as practicable after the effective date of this registration
statement.
If
any of
the securities being registered on this Form are to be offered on a delayed
or
continuous basis pursuant to Rule 415 under the Securities Act of 1933, as
amended, check the following box. Q
If
this
Form is filed to register additional securities for an offering pursuant to
Rule
462(b) under the Securities Act, check the following box and list the Securities
Act registration statement number of the earlier effective registration
statement for the same offering. £
If
this
Form is a post-effective amendment filed pursuant to Rule 462(c) under the
Securities Act, check the following box and list the Securities Act registration
statement number of the earlier effective registration statement for the same
offering. £
If
this
form is a post-effective amendment filed pursuant to Rule 462(d) under the
Securities Act, check the following box and list the Securities Act registration
statement number of the earlier effective registration statement for the same
offering. £
If
delivery of the prospectus is expected to be made pursuant to Rule 434, please
check the following box. £
CALCULATION
OF REGISTRATION FEE
|
Title
of Each Class of Securities to be Registered(1)
|
Amount
to
be
Registered
|
Proposed
Maximum
Aggregate
Offering
Price
|
Amount
of
Registration
Fee
|
|||||||
|
Ordinary
Shares, par value NIS 0.02
|
46,666,670
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$
|
31,360,002(2
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)
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$
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3,356 | ||||
|
Ordinary
Shares, par value NIS 0.02
|
23,333,335(3
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)
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$
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20,416,668(4
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)
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$
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2,184
|
|||
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(1)
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A
separate registration statement on Form F−6 (Registration No. 333−12696)
has been filed for the registration of American Depositary Shares
evidenced by American Depositary Receipts issuable upon the deposit
of
ordinary shares registered hereby. Each American Depositary Share
represents ten ordinary shares.
|
|
(2)
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Estimated
solely for the purposes of computing the amount of the registration
fee
pursuant to Rule 457(c) under the Securities Act based on the average
of
the high and low prices of the American Depositary Shares, divided
by the
ten ordinary shares represented thereby, reported on the Nasdaq
National
Market on April 19, 2006.
|
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(3)
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Issuable
upon exercise of warrants issued to the Selling
Shareholders.
|
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(4)
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Estimated
solely for the purposes of computing the amount of the registration
fee
pursuant to Rule 457(g) under the Securities Act, and is $20,416,668,
the
exercise price of the warrants issued to the Selling
Shareholders.
|
The
registrant hereby amends this registration statement on such date or dates
as
may be necessary to delay its effective date until the registrant shall file
a
further amendment which specifically states that this registration statement
shall thereafter become effective in accordance with Section 8(a) of the
Securities Act of 1933 or until this registration statement shall become
effective on such date as the Commission, acting pursuant to said Section 8(a),
may determine.
The
information in this prospectus is not complete and
may be changed. We may not sell these securities until the registration
statement filed with the Securities and Exchange Commission is effective.
This
prospectus is not an offer to sell these securities and it is not soliciting
an
offer to buy these securities in any state where the offer or sale is not
permitted.
Subject to Completion, dated April 20,
2006.PROSPECTUS
7,000,000.5
American Depositary Shares
Representing
Ten Ordinary Shares
XTL
Biopharmaceuticals Ltd.
________________
This
prospectus relates to the offer and sale by the Selling Shareholders named
herein of up to an aggregate of 70,000,005 ordinary shares in the form of
American Depositary Shares, or ADSs, which we refer to herein as “Shares,” of
XTL Biopharmaceuticals Ltd., an Israeli public limited liability company. Each
ADS represents ten ordinary shares. The ADSs are evidenced by American
Depositary Receipts, or ADRs. The number of ordinary shares being offered
includes 23,333,335 ordinary shares, which are issuable upon the exercise of
warrants, and which we refer to herein as “Warrant Shares.” The Selling
Shareholders may, from time to time, sell any or all of their ADRs on the Nasdaq
Stock Market or in private transactions using any of the methods described
in
the section of this prospectus entitled “Plan of Distribution.” We will not
receive any proceeds from the sale of the ADRs by the Selling Shareholders
other
than the exercise price payable to us upon the exercise of the warrants. We
issued these ordinary shares to the Selling Shareholders in a private
transaction.
Our
ordinary shares are traded on the London Stock Exchange under the symbol “XTL”
and on the Tel Aviv Stock Exchange under the symbol “XTL.” ADRs representing our
ordinary shares are quoted on the Nasdaq Stock Market under the symbol
“XTLB.”
On
April 19, 2006, the closing price of our ordinary shares on the London Stock
Exchange was 37.25 British Pence per share, the closing price of our ordinary
shares on the Tel Aviv Stock Exchange was NIS 3.159 per share, and the closing
price of our ADRs on the Nasdaq Stock Market was $6.72 per ADR.
Investing
in our ADRs involves risks. See “Risk Factors” beginning on page 9.
________________
Neither
the Securities and Exchange Commission nor any state securities commission
has
approved or disapproved these securities, or determined if this prospectus
is
truthful or complete. Any representation to the contrary is a criminal
offense.
________________
The
date
of this prospectus is , 2006.
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8
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F-1
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________________
You
should rely only on the information contained in this prospectus. We have not
authorized anyone to provide you with information different from that contained
in this prospectus. This prospectus may be used only where it is legal to sell
these securities. You should not assume that the information in this prospectus
is accurate as of any date other than the date on the front of this prospectus.
Our business, financial condition, results of operations and prospects may
have
changed since then.
The
following is a summary of selected information contained elsewhere in this
prospectus. It does not contain all of the information that you should consider
before deciding to invest in our ordinary shares or ADRs. You should read this
entire prospectus carefully, especially the section entitled “Risk Factors” and
the financial statements and the notes to the financial statements at the end
of
the prospectus. Unless the context requires otherwise, references in this
prospectus to “XTLbio,” the “Company,” “we,” “us” and “our” refer to XTL
Biopharmaceuticals Ltd. and our wholly-owned subsidiary, XTL Biopharmaceuticals,
Inc. We have prepared our consolidated financial statements in United States
dollars and in accordance with United States generally accepted accounting
principles, or U.S. GAAP. All references herein to "dollars" or "$" are to
United States dollars, and all references to "Shekels" or "NIS" are to New
Israeli Shekels.
XTL
Biopharmaceuticals Ltd.
Company
Information
We
are a
biopharmaceutical company engaged in the acquisition, development and
commercialization of pharmaceutical products for the treatment of infectious
diseases, particularly the treatment of hepatitis C. We are developing XTL-2125,
a small molecule non-nucleoside, polymerase inhibitor for the treatment of
patients with hepatitis C. XTL-2125 is expected to commence a Phase I clinical
trial in patients with chronic hepatitis C in the first half of 2006. A second
drug candidate, XTL-6865, is also being developed for the treatment of patients
with hepatitis C. XTL-6865 is a combination of two monoclonal antibodies against
the hepatitis C virus. The antibodies comprising XTL-6865 are expected to “trap”
the virus in the patient’s serum and prevent the infection of healthy liver
cells. In September 2005, we announced the initiation of a Phase Ia clinical
trial with XTL-6865 in patients with chronic hepatitis C. Our third program
in
the hepatitis C area is the Diversity Oriented Synthesis, or DOS, program.
This
program is focused on the development of novel hepatitis C small molecule
inhibitors. These compounds are presently being optimized. We expect to identify
the first clinical candidate from the DOS program and start IND-enabling
GLP-safety studies with this clinical candidate in the second half of 2006.
Another product under development, HepeX-B, is designed to prevent re-infection
with hepatitis B in liver transplant patients, and was recently studied in
a
Phase IIb trial in liver transplant patients. Worldwide rights for HepeX-B
were
licensed to Cubist Pharmaceuticals Inc., or Cubist, in exchange for certain
milestone payments and future royalties on Cubist’s net sales. In December 2005,
data from the Phase IIb trial in liver transplant patients showed that patients
treated with HepeX-B experienced no evidence of viral reinfection. Cubist
recently met with the FDA to discuss proposed changes to the method of
manufacture and formulation of HepeX-B. Cubist will meet again with the FDA
in
the first half of 2006 to discuss the implications of these changes on the
next
stage of the clinical program.
Our
legal
and commercial name is XTL Biopharmaceuticals Ltd. We were established as a
private company limited by shares under the laws of the State of Israel on
March
9, 1993, under the name Xenograft Technologies Ltd. We re-registered as a public
company on June 7, 1993, in Israel, and changed our name to XTL
Biopharmaceuticals Ltd. on July 3, 1995. We commenced operations to use and
commercialize technology developed at the Weizmann Institute, in Rehovot,
Israel. Until 1999, our therapeutic focus was on the development of human
monoclonal antibodies to treat viral, autoimmune and oncological diseases.
Our
first therapeutic programs focused
on
antibodies against the hepatitis B virus, interferon - γ and the hepatitis C
virus.
Our
ordinary shares are traded on the London Stock Exchange under the symbol “XTL,”
and on the Tel Aviv Stock Exchange under the symbol “XTL.” Our ADRs are quoted
on the Nasdaq Stock Market under the symbol “XTLB.”
We
operate under the laws of the State of Israel, under the Israeli Companies
Act
and the regulations of the United Kingdom Listing Authority, which governs
our
listing on the London Stock Exchange.
Our
principal offices are located at 750 Lexington Avenue, 20th
Floor,
New York, New York 10022 and our telephone number is 212-531-5960. The principal
offices of XTL Biopharmaceuticals, Inc., our wholly-owned U.S. subsidiary and
agent for service of process in the U.S., are located at 750 Lexington Avenue,
20th
Floor,
New York, NY 10022, and its telephone number is 212-531-5960. Our primary
internet address is www.xtlbio.com. None of the information on our website
is
incorporated by reference into this registration statement.
The
Offering
|
Securities
offered hereby:
|
46,666,670 ordinary shares, par value NIS 0.02 per share, in the form of ADRs, and 23,333,335 ordinary shares underlying warrants, also in the form of ADRs. | |
|
Use
of proceeds:
|
Except for proceeds, if any, received in connection with the exercise of warrants, we will not receive any proceeds from the sale of ADRs by the Selling Shareholders. Any proceeds received in connection with the exercise of warrants will be used for general corporate purposes. | |
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ADRs:
|
Each ADR represents the right to receive ten ordinary shares. See "Description of American Depositary Shares." | |
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||
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·
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The
depositary will hold the shares underlying your ADRs. You will have
rights
as provided in the deposit agreement.
|
|
|
·
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We
do not expect to pay dividends in the foreseeable future. If, however,
we
declare dividends on our ordinary shares, the depositary will pay
you the
cash dividends and other distributions it receives on our ordinary
shares,
after deducting its fees and expenses.
|
|
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·
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You
may turn in your ADRs to the depositary in exchange for our ordinary
shares. The depositary will charge you fees for any such
exchange.
|
|
|
·
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We
may amend or terminate the deposit agreement without your consent.
If you
continue to hold your ADRs, you agree to be bound by the deposit
agreement, as amended.
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Depositary:
|
The Bank of New York | |
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Timing
and Settlement for ADRs:
|
The ADRs will be deposited with a custodian for, and registered in the name of a nominee of, The Depository Trust Company, or DTC, in New York, New York. DTC and its direct and indirect participants will maintain records that will show the beneficial interests in the ADRs and facilitate any transfer of the beneficial interests. | |
|
Nasdaq
Stock Market symbol for ADRs:
|
“XTLB” | |
The
following table presents our summary financial data for the dates and periods
indicated. This data should be read together with “Management’s Discussion and
Analysis of Financial Condition and Results of Operations.” We have derived the
selected financial data for the fiscal years ended December 31, 2005, 2004
and
2003, and as of December 31, 2005 and 2004, which have prepared in accordance
with U.S. GAAP from our audited consolidated financial statements,
included with this prospectus. We have derived the selected financial data
for
fiscal years ended December 31, 2002 and 2001, and as of December 31, 2003,
2002
and 2001, from audited consolidated financial statements not appearing in this
prospectus, which have been prepared in accordance with U.S.
GAAP.
|
Year
Ended December 31,
|
||||||||||||||||
|
2005
|
2004
|
2003
|
2002
|
2001
|
||||||||||||
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(In
thousands, except per share amounts)
|
|||||||||||||||
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Statements
of Operations Data:
|
||||||||||||||||
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Revenues
|
|
|
|
|
||||||||||||
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Reimbursed
out of pocket expenses
|
$
|
2,743
|
$
|
3,269
|
$
|
--
|
$
|
--
|
$
|
--
|
||||||
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License
|
454
|
185
|
--
|
--
|
--
|
|||||||||||
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3,197
|
3,454
|
--
|
--
|
--
|
||||||||||||
|
Cost
of Revenues
|
|
|
|
|
||||||||||||
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Reimbursed
out of pocket expenses
|
2,743
|
3,269
|
--
|
--
|
--
|
|||||||||||
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License
|
54
|
32
|
--
|
--
|
--
|
|||||||||||
|
2,797
|
3,301
|
|
|
|
||||||||||||
|
Gross
Margin
|
400
|
153
|
--
|
--
|
--
|
|||||||||||
|
|
|
|
|
|
|
|||||||||||
|
Research
and development
|
|
|
|
|
|
|||||||||||
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Research
and development costs
|
7,313
|
11,985
|
14,022
|
13,231
|
12,187
|
|||||||||||
|
Less
participations
|
--
|
--
|
3,229
|
75
|
1,133
|
|||||||||||
|
|
7,313
|
11,985
|
10,793
|
13,156
|
11,054
|
|||||||||||
|
In-process
research and development
|
1,783
|
--
|
--
|
--
|
--
|
|||||||||||
|
General
and administrative
|
5,457
|
4,134
|
3,105
|
3,638
|
3,001
|
|||||||||||
|
Business
development costs
|
227
|
810
|
664
|
916
|
1,067
|
|||||||||||
|
|
|
|
|
|||||||||||||
|
Operating
loss
|
(14,380
|
)
|
(16,776
|
)
|
(14,562
|
)
|
(17,710
|
)
|
(15,122
|
)
|
||||||
|
|
|
|
||||||||||||||
|
Other
income (expense)
|
|
|
|
|
||||||||||||
|
Financial
income, net
|
443
|
352
|
352
|
597
|
2,448
|
|||||||||||
|
Taxes
on income
|
(78
|
)
|
(49
|
)
|
(78
|
)
|
(27
|
)
|
--
|
|||||||
|
|
|
|
|
|
||||||||||||
|
Net
loss
|
$
|
(14,015
|
)
|
$
|
(16,473
|
)
|
$
|
(14,288
|
)
|
$
|
(17,140
|
)
|
$
|
(12,674
|
)
|
|
|
|
|
|
||||||||||||||
|
Net
loss per ordinary share
|
|
|
||||||||||||||
|
Basic
and diluted
|
$
|
(0.08
|
)
|
$
|
(0.12
|
)
|
$
|
(0.13
|
)
|
$
|
(0.15
|
)
|
$
|
(0.11
|
)
|
|
|
Weighted
average shares outstanding
|
170,123,003
|
134,731,766
|
111,712,916
|
111,149,292
|
110,941,014
|
|||||||||||
|
As
of December 31,
|
||||||||||||||||
|
|
2005
|
|
|
2004
|
|
|
2003
|
|
|
2002
|
|
|
2001
|
|||
|
|
(In
thousands, except per share amounts)
|
|||||||||||||||
|
Balance
Sheet Data:
|
||||||||||||||||
|
Cash,
cash equivalents, bank deposits and
marketable
securities
|
$
|
13,360
|
$
|
22,924
|
$
|
22,262
|
$
|
35,706
|
$
|
52,188
|
||||||
|
Working
capital
|
11,385
|
20,240
|
19,967
|
33,396
|
50,433
|
|||||||||||
|
Total
assets
|
15,151
|
25,624
|
24,853
|
38,423
|
55,106
|
|||||||||||
|
Long-term
obligations
|
1,493
|
2,489
|
1,244
|
1,017
|
526
|
|||||||||||
|
Total
shareholders’ equity
|
11,252
|
19,602
|
20,608
|
34,830
|
51,953
|
|||||||||||
Recent
Developments
Private
Placement
On
March
22, 2006, we completed a private placement of 46,666,670 ordinary shares
(equivalent to 4,666,667 ADRs) at $0.60 per share ($6.00 per ADR), together
with
warrants for the purchase of an aggregate of 23,333,335 ordinary shares
(equivalent to 2,333,333.5 ADRs) at an exercise price of $0.875 ($8.75 per
ADR),
for an aggregate consideration of approximately $28 million in gross proceeds.
In
connection with the private placement, we have agreed not to issue or sell
any
ordinary shares or ADRs, excluding the issuance of ordinary shares or ADRs
representing ordinary shares issued upon the exercise of currently outstanding
options and warrants, prior to the effective date of the registration statement
of which this prospectus is a part.
We
plan
to use the net proceeds from the private placement for the further development
of our clinical-stage drug candidates, the development of our pre-clinical
stage
compounds to identify a clinical candidate for IND enabling GLP safety studies,
the potential in-license or acquisition of additional drug candidates, and
for
general corporate purposes.
Warrants
The
warrants issued as part of the private placement have an exercise price of
$0.875, equivalent to $8.75 per ADR, subject to adjustments in connection with
dividends on our ordinary shares, and subdivisions, combinations and
reclassifications of our ordinary shares. The warrants have a term of exercise
of five years.
If
we
complete a reorganization, reclassification, merger, consolidation or
disposition of assets, then the holders of the warrants shall have the right
thereafter to receive upon exercise of the warrants, the number of shares of
common stock of the successor or acquiring corporation and other property
receivable upon or as a result of such reclassification, merger, consolidation
or disposition of assets by a holder of the number of ordinary shares for which
the warrants are exercisable immediately prior to such event.
We
may at
any time during the term of the warrant reduce the then current exercise price
to any amount and for any period of time deemed appropriate by our board of
directors; provided, however, that we give notice to the holder, which notice
shall state the number of warrant shares (and other securities or property)
purchasable upon the exercise of the warrant and the exercise price of such
warrant after such adjustment, setting forth a brief statement of the facts
requiring such adjustment and setting forth the computation by which such
adjustment was made.
Registration
Rights
We
entered into a registration rights agreement with the Selling Shareholders
on
March 22, 2006. The registration rights agreement provides that we must file
a
registration statement on or prior to the 30th
day
following March 22, 2006, covering the resale of all of our ordinary shares
sold
by us in the private placement and all of our ordinary shares issuable upon
exercise of the warrants issued to the Selling Shareholders as part of the
private placement. This prospectus is part of the registration statement filed
to meet our obligations under the registration rights agreement.
We
must
cause this registration statement to become effective as soon as practicable,
but in no event later than the 90th calendar day, or 105th calendar day in
the
event of a full review by the SEC, following March 22, 2006. If this
registration statement is not declared effective by the SEC on or before the
90th day, or 105th day, if applicable, registration deadline, or if after this
registration statement has been declared effective by the SEC, sales of the
ADRs
representing ordinary shares covered by the registration statement cannot be
made pursuant to this registration statement for any reason, then at the time
of
the event, we are required to make payments to the Selling Shareholders in
the
amount of 2.0% per month of the aggregate purchase price paid in the private
placement by the Selling Shareholders for the ADRs representing our ordinary
shares held by the Selling Shareholders. If we fail to make this payment within
seven days after the date payable, we will pay interest at a rate of 15% per
annum (or such lesser maximum amount that is permitted to be paid by applicable
law) to the holder.
VivoQuest
- Unaudited Pro Forma Financial Information
In
September 2005, we licensed from VivoQuest, Inc., a U.S. privately-held company
which is a development stage enterprise, exclusive worldwide rights to
VivoQuest’s intellectual property and technology, covering a proprietary
compound library, including VivoQuest’s lead hepatitis C compounds. In addition,
we acquired from VivoQuest certain assets, including VivoQuest’s laboratory
equipment, assumed VivoQuest’s lease of its laboratory space and certain
research and development employees.
In
connection with the VivoQuest transaction, we:
|
(1)
|
issued
1,314,420 of our ordinary shares with an aggregate value of $1,391,000
(calculated based upon the average of the closing prices per share
for the
period commencing two days before, and ending two days after, the
closing
of the transaction);
|
|
(2)
|
paid
approximately $400,000 to VivoQuest to fund certain of their operating
expenses prior to the closing of the transaction, and incurred $148,000
in
direct expenses associated with the transaction;
|
|
(3)
|
agreed
to make additional contingent milestone payments triggered by certain
regulatory and sales targets, totaling up to $34.6 million, $25.0
million
of which will be due upon or following regulatory approval or actual
product sales, which are payable in cash or ordinary shares at our
election (no contingent consideration has been paid pursuant to the
license agreement as of the balance sheet date, because none of the
milestones have been achieved - the contingent consideration will
be
recorded as part of the acquisition costs in the future); and
|
|
(4)
|
agreed
to make royalty payments on future product
sales.
|
As
VivoQuest is a development stage enterprise that had not yet commenced its
planned principal operations, we accounted for the transaction as an acquisition
of assets pursuant to the provisions of Statement of Financial Accounting
Standards No. 142 “Goodwill and Other Intangible Assets,” or FAS 142.
Accordingly, the purchase price was allocated to the individual assets acquired,
based on their estimated fair values, and no goodwill was recorded.
The
purchase price consisted of:
|
($
in thousands)
|
||||
|
Fair
value of XTLbio’s ordinary shares
|
$ |
1,391
|
||
|
Cash
consideration paid
|
400
|
|||
|
Direct
expenses associated with the VivoQuest transaction
|
148
|
|||
|
Total
purchase price
|
$ |
1,939
|
||
The
tangible and intangible assets acquired consisted of the following:
|
($
in thousands)
|
||||
|
Tangible
assets acquired - property and equipment
|
$ |
113
|
||
|
Intangible
assets acquired:
|
||||
|
In-process
research and development
|
1,783
|
|||
|
Assembled
workforce
|
43
|
|||
|
Total
intangible assets acquired
|
1,826
|
|||
|
Total
tangible and intangible assets acquired
|
$ |
1,939
|
||
The
amount allocated to in-process research and development represents the estimated
fair value of purchased in-process research and development that, as of the
transaction date, have not reached technological feasibility and have no proven
alternative future use. Accordingly, they were charged in the consolidated
statement of operations as “in- process research and development
costs.”
The
assembled workforce that was acquired is being amortized using the straight-line
method over its estimated useful life of three years, and is classified as
“intangible assets” on our balance sheet.
The
following unaudited pro forma financial information presents the combined
results of operations of XTLbio and VivoQuest as if the VivoQuest transaction
had occurred as of January 1, 2005. The unaudited pro forma financial
information is not necessarily indicative of what our consolidated results
of
operations actually would have been had we completed the transaction on the
dates indicated. In addition, the unaudited pro forma financial information
does
not purport to project our future results of operations.
XTL
Biopharmaceuticals Ltd.
Unaudited
Proforma Condensed Statement of Operations
For
the
Year Ended December 31, 2005
($
in
thousands, except share and per share amounts)
|
|
Historical
XTLbio
|
Historical
VivoQuest1
|
Pro
forma
adjustments
|
Pro
forma
combined
|
|||||||||
|
Revenues
|
$ |
3,197
|
--
|
--
|
$ |
3,197
|
|||||||
|
Cost
of revenues
|
2,797
|
--
|
--
|
2,797
|
|||||||||
|
Gross
margin
|
400
|
--
|
--
|
400
|
|||||||||
|
Research
and development
|
7,313
|
2,186
|
623(a)(b
|
)
|
10,122
|
||||||||
|
In-process
research and development
|
1,783
|
--
|
(1,783)(c
|
)
|
--
|
||||||||
|
General
and administrative
|
5,457
|
740
|
70(b
|
)
|
6,267
|
||||||||
|
Business
development
|
227
|
--
|
--
|
227
|
|||||||||
|
Depreciation
and amortization
|
--
|
282
|
(282)(b
|
)
|
--
|
||||||||
|
Operating
loss
|
(14,380
|
)
|
(3,208
|
)
|
|
(16,216
|
)
|
||||||
|
Other
income (expense)
|
|||||||||||||
|
Financial
income, net
|
443
|
(342
|
)
|
358(d
|
)
|
459
|
|||||||
|
Dividends
on preferred stock
|
--
|
(1,108
|
)
|
1,108(e
|
)
|
|
|||||||
|
Taxes
on income
|
(78
|
)
|
--
|
(78
|
)
|
||||||||
|
Net
loss
|
$ |
(14,015
|
)
|
(4,568
|
)
|
|
$ |
(15,835
|
)
|
||||
|
Net
loss per ordinary share
|
(0.08
|
)
|
(0.09
|
)
|
|||||||||
|
Weighted
average shares outstanding
|
170,123,003
|
947,102(f |
)
|
171,070,105
|
|||||||||
1
Until
completion of the transaction in September 2005.
The
following pro forma adjustments have been made to the unaudited proforma
condensed statement of operations:
|
|
(a)
|
An
amount of $400,000 representing the interim funding provided by XTLbio
to
VivoQuest which reduced VivoQuest’s research and development costs has
been eliminated (the amount has been included in in-process research
and
development in our historical financial statements). In addition,
an
amount of $11,000 has been included to account for the amortization
of the
assembled workforce, as if the transaction had occurred on January
1,
2005.
|
|
|
(b)
|
VivoQuest’s
historical depreciation and amortization expense of $282,000 has
been
allocated between research and development ($212,000) and general
and
administrative ($70,000).
|
|
|
(c)
|
The
one-time charge of $1,783,000 to expense for the fair value of the
in-process research and development has been excluded from the unaudited
pro forma condensed combined consolidated statement of operations
due to
its non-recurring nature.
|
|
|
(d)
|
Interest
expense of $358,000 related to VivoQuest’s convertible debentures, that
were not assumed, has been eliminated.
|
|
|
(e)
|
Dividends
on preferred stock of $1,018,000, that were not assumed, have been
eliminated.
|
|
(f)
|
An
amount of 947,102 ordinary shares have been added to the weighted
average
shares outstanding to present the weighted average shares outstanding
as
if the transaction had occurred on January 1,
2005.
|
Certain
matters discussed in this report, including matters discussed under the caption
“Management’s Discussion and Analysis of Financial Condition and Results of
Operations,” may constitute forward-looking statements for purposes of the
Securities Act of 1933, as amended, or the Securities Act, and the Securities
Exchange Act of 1934, as amended, or the Exchange Act, and involve known and
unknown risks, uncertainties and other factors that may cause our actual
results, performance or achievements to be materially different from the future
results, performance or achievements expressed or implied by such
forward-looking statements. The words “expect,” “anticipate,” “intend,” “plan,”
“believe,” “seek,” “estimate,” and similar expressions are intended to identify
such forward-looking statements. Our actual results may differ materially from
the results anticipated in these forward-looking statements due to a variety
of
factors, including, without limitation, those discussed under “Risks Factors”
and elsewhere in this report, as well as factors which may be identified from
time to time in our other filings with the Securities and Exchange Commission,
or the SEC, or in the documents where such forward-looking statements appear.
All written or oral forward-looking statements attributable to us are expressly
qualified in their entirety by these cautionary statements.
The
forward-looking statements contained in this report reflect our views and
assumptions only as of the date this report is signed. Except as required by
law, we assume no responsibility for updating any forward-looking statements.
8
Before
you invest in our ordinary shares or ADRs, you should understand the high degree
of risk involved. You should carefully consider the risks described below and
other information in this prospectus, including our financial statements and
related notes included elsewhere in this prospectus, before you decide to
purchase our ordinary shares or ADRs. If any of the following risks
actually
occur, our business, financial condition and operating results could be
adversely affected. As a result, the trading price of our
ordinary shares or ADRs could decline and you could lose part or all of your
investment.
Risks
Related to Our Business
We
have a limited operating history and have incurred substantial operating losses
since our inception. We expect to continue to incur losses in the future and
may
never become profitable.
We
have a
limited operating history. You should consider our prospects in light of the
risks and difficulties frequently encountered by development stage companies.
In
addition, we have incurred operating losses since our inception and expect
to
continue to incur operating losses for the foreseeable future. As of December
31, 2005, we had an accumulated deficit of approximately $100 million. We may
continue to incur substantial operating losses even if we begin to generate
revenues from our drug candidates or technologies. Consequently, if those
revenues are insufficient to cover development and other expenditures we may
incur, we may never become profitable.
We
have not received approval for the sale of any of our products in any market
and, therefore, have not generated any commercial revenues from the sales of
our
products. We have relied on equity financings to fund our
operations.
We
have
not yet commercialized any of our drug candidates or technologies and cannot
be
sure we will ever be able to do so. Even if we commercialize one or more of
our
drug candidates or technologies, we may not become profitable. Our ability
to
achieve profitability depends on a number of factors, including our ability
to
complete our development efforts, obtain regulatory approval for our drug
candidates and technologies and successfully commercialize them. Moreover,
we
have relied on equity financings to fund our operations, and we expect to use,
rather than generate, funds from operations for the foreseeable future. See
“-
Risks Related to our Financial Condition” below.
If
we are unable to successfully complete our clinical trial programs for our
drug
candidates, or if such clinical trials take longer to complete than we project,
our ability to execute our current business strategy will be adversely affected.
Whether
or not and how quickly we complete clinical trials is dependent in part upon
the
rate at which we are able to engage clinical trial sites and, thereafter, the
rate of enrollment of patients. Patient enrollment is a function of many
factors, including the size of the patient population, the proximity of patients
to clinical sites, the eligibility criteria for the study and the existence
of
competitive clinical trials. If we experience delays in identifying and
contracting with sites and/or in patient enrollment in our clinical trial
programs, we may incur additional costs and delays in our development programs
and may not be able to complete our clinical trials on a cost-effective basis.
If
third parties on which we rely for clinical trials do not perform as
contractually required or as we expect, we may not be able to obtain regulatory
approval for or commercialize our products.
We
depend
on independent clinical investigators, contract research organizations and
other
third-party service providers to conduct the clinical trials of our drug
candidates and technologies and expect to continue to do so. We rely heavily
on
these parties for successful execution of our clinical trials, but we do not
control many aspects of their activities. Nonetheless, we are responsible for
confirming that each of our clinical trials is conducted in accordance with
the
general investigational plan and protocol. Our reliance on these third parties
that we do not control does not relieve us of our responsibility to comply
with
the regulations and standards of the U.S. Food and Drug Administration, or
the
FDA, relating to good clinical practices. Third parties may not complete
activities on schedule or may not conduct our clinical trials in accordance
with
regulatory requirements or the applicable trial’s plans and protocols. The
failure of these third parties to carry out their obligations could delay or
prevent the development, approval and commercialization of our products or
result in enforcement action against us.
If
the clinical data related to our drug candidates and technologies do not confirm
positive early clinical data or preclinical data, our corporate strategy and
financial results will be adversely impacted.
All
of
our drug candidates and technologies are in preclinical or clinical stages.
Specifically, one of our drug candidates, HepeX-B, was recently studied in
a
Phase IIb trial, XTL-6865 is currently in a Phase I clinical trial and two
of
our programs under development, XTL-2125 and DOS, have not yet been tested
in
humans. In order for our candidates to proceed to later stage clinical testing,
they must show positive preclinical or clinical data. While HepeX-B, XTL-6865
and XTL-2125 have shown promising preclinical data and HepeX-B has shown
promising clinical data, preliminary results of pre-clinical or clinical tests
do not necessarily predict the final results, and promising results in
pre-clinical or early clinical testing might not be obtained in later clinical
trials. Drug candidates in the later stages of clinical development may fail
to
show the desired safety and efficacy traits despite having progressed through
initial clinical testing. Any negative results from future tests may prevent
us
from proceeding to later stage clinical testing which would materially impact
our corporate strategy and our financial results may be adversely impacted.
We
have limited experience in conducting and managing clinical trials necessary
to
obtain regulatory approvals. If
our drug candidates and technologies do not receive the necessary regulatory
approvals, we will be unable to commercialize our products.
We
have
not received, and may never receive, regulatory approval for commercial sale
for
any of our products. We currently do not have any drug candidates or
technologies pending approval with the FDA or with regulatory authorities of
other countries. We will need to conduct significant additional research and
human testing before we can apply for product approval with the FDA or with
regulatory authorities of other countries. Pre-clinical testing and clinical
development are long, expensive and uncertain processes. Satisfaction of
regulatory requirements typically depends on the nature, complexity and novelty
of the product and requires the expenditure of substantial resources. Regulators
may not interpret data obtained from pre-clinical and clinical tests of our
drug
candidates and technologies the same way that we do, which could delay, limit
or
prevent our receipt of regulatory approval. It may take us many years to
complete the testing of our drug candidates and technologies, and failure can
occur at any stage of this process. Negative or inconclusive results or medical
events during a clinical trial could cause us to delay or terminate our
development efforts.
Clinical
trials also have a high risk of failure. A number of companies in the
pharmaceutical industry, including biotechnology companies, have suffered
significant setbacks in advanced clinical trials, even after achieving promising
results in earlier trials. If we experience delays in the testing or approval
process or if we need to perform more or larger clinical trials than originally
planned, our financial results and the commercial prospects for our drug
candidates and technologies may be materially impaired. In addition, we have
limited experience in conducting and managing the clinical trials necessary
to
obtain regulatory approval in the United States and abroad and, accordingly,
may
encounter unforeseen problems and delays in the approval process.
Even
if
regulatory approval is obtained, our products and their manufacture will be
subject to continual review, and there can be no assurance that such approval
will not be subsequently withdrawn or restricted. Changes in applicable
legislation or regulatory policies, or discovery of problems with the products
or their manufacture, may result in the imposition of regulatory restrictions,
including withdrawal of the product from the market, or result in increased
costs to us.
Because
we license some of our proprietary technologies from third-parties, some of
these third-parties could prevent us from licensing our drug candidates.
We
do not
own all of our drug candidates and technologies. We have licensed the patent
rights to some of our drug candidates and/or the technologies on which they
are
based from others. Specifically, we have licensed the two human monoclonal
antibodies comprising XTL-6865 from Stanford University and DRK-Blutspendedienst
Baden-Wurttemberg, we have licensed XTL-2125 from B&C Biopharm Co. Ltd., and
we have licensed certain other Hepatitis C virus, or HCV, compounds from
VivoQuest Inc., or VivoQuest. We have also licensed the Trimera technology
upon
which certain of our current programs are based from the Yeda Research and
Development Company Ltd., which we refer to as Yeda. These license agreements
require us to meet development or financing milestones and impose development
and commercialization due diligence requirements on us. In addition, under
these
agreements, we must pay royalties on sales of products resulting from licensed
drugs and technologies and pay the patent filing, prosecution and maintenance
costs related to the licenses. While we have the right to defend patent rights
related to our licensed drug candidates and technologies, we are not obligated
to do so. In the event that we decide to defend our licensed patent rights,
we
will be obligated to cover all of the expenses associated with that effort.
If we do not meet our obligations in a timely manner or if we otherwise breach
the terms of our agreements, our licensors could terminate the agreements,
and
we would lose the rights to our drug candidates and technologies. For a further
discussion on our license agreements, the patent rights related to those
licenses, and the expiration dates of those patent rights, see “Business -
Business Overview - Intellectual Property and Patents” and “Business - Business
Overview - Licensing Agreements and Collaborations” below. In addition, see “-
Risks Related to Our Intellectual Property” below regarding potential issues
related to the use of patents owned by third-parties.
In
addition, under the terms of our license agreement with Yeda, we are required
to
obtain their approval under the license in order to grant sub-licenses to
collaborative partners to develop or commercialize products or products derived
from technologies under the license. The requirement of obtaining these
approvals, and any conditions that Yeda may impose upon such approvals, could
have the effect of delaying or impeding our ability to enter into agreements
with collaborative partners or result in our having to accept terms and
conditions that might not be favorable to us. For a discussion of further
required approvals, see “- Risks Relating to Operations in Israel” below
regarding potential restrictions from the Office of the Chief Scientist
regarding the manufacture of our drug candidates outside the State of
Israel.
If
we do not establish or maintain drug development and marketing arrangements
with
third parties, we may be unable to commercialize our drug candidates and
technologies into products.
We
are an
emerging company and do not possess all of the capabilities to fully
commercialize our drug candidates and technologies on our own. From time to
time, we may need to contract with third parties to:
|
·
|
assist
us in developing, testing and obtaining regulatory approval for some
of
our compounds and technologies;
|
|
·
|
manufacture
our drug candidates; and
|
|
·
|
market
and distribute our products.
|
We
can
provide no assurance that we will be able to successfully enter into agreements
with such third-parties on terms that are acceptable to us. If we are unable
to
successfully contract with third parties for these services when needed, or
if
existing arrangements for these services are terminated, whether or not through
our actions, or if such third parties do not fully perform under these
arrangements, we may have to delay, scale back or end one or more of our drug
development programs or seek to develop or commercialize our drug candidates
and
technologies independently, which could result in delays. Further, such failure
could result in the termination of license rights to one or more of our drug
candidates and technologies. Moreover, if these development or marketing
agreements take the form of a partnership or strategic alliance, such
arrangements may provide our collaborators with significant discretion in
determining the efforts and resources that they will apply to the development
and commercialization of our products. Accordingly, to the extent that we rely
on third parties to research, develop or commercialize our products, we are
unable to control whether such products will be scientifically or commercially
successful.
For
example, in June 2004, we announced the completion of a license agreement with
Cubist Pharmaceuticals, Inc., or Cubist, for the worldwide development and
commercialization of HepeX-B. Under this agreement, we were responsible for
certain clinical and product development activities of HepeX-B through August
2005, at the expense of Cubist. Thereafter, we transferred full responsibility
for completing the development of HepeX-B to Cubist. Cubist will be responsible
for completing the development and for registration and commercialization of
the
product worldwide. Accordingly, to a significant degree, we are unable to
control whether HepeX-B will be scientifically or commercially successful.
In
addition, Cubist recently met with the FDA to discuss proposed changes to the
method of manufacture and formulation of HepeX-B. The objective of the
manufacturing change is to provide a stable platform for commercialization.
Cubist will meet again with the FDA in the first-half of 2006 to discuss the
implications of these changes on the next stage of the clinical program. There
can be no assurance that they will be successful in developing HepeX-B for
commercialization, and, as a result, no assurance that we will receive any
proceeds from the sale of HepeX-B.
If
our products fail to achieve market acceptance, we will never record meaningful
revenues.
Even
if
our products are approved for sale, they may not be commercially successful
in
the marketplace. Market acceptance of our product candidates will depend on
a
number of factors, including:
|
·
|
perceptions
by members of the health care community, including physicians, of
the
safety and efficacy of our products;
|
|
·
|
the
rates of adoption of our products by medical practitioners and the
target
populations for our products;
|
|
·
|
the
potential advantages that our products offer over existing treatment
methods or other products that may be developed;
|
|
·
|
the
cost-effectiveness of our products relative to competing products;
|
|
·
|
the
availability of government or third-party payor reimbursement for
our
products;
|
|
·
|
the
side effects or unfavorable publicity concerning our products or
similar
products; and
|
|
·
|
the
effectiveness of our sales, marketing and distribution efforts.
|
Because
we expect sales of our products to generate substantially all of our revenues
in
the long-term, the failure of our products to find market acceptance would
harm
our business and could require us to seek additional financing or other sources
of revenue.
If
the third parties upon whom we rely to manufacture our products do not
successfully manufacture our products, our business will be harmed.
We
do not
currently have the ability to manufacture ourselves the compounds that we need
to conduct our clinical trials and rely upon a limited number of manufacturers
to supply our drug candidates. We have no experience in manufacturing compounds
for clinical or commercial purposes and do not have any manufacturing
facilities. We rely upon, and intend to continue to rely upon, third parties
to
manufacture our drug candidates for use in clinical trials and for future sales.
In order to commercialize our products, such products will need to be
manufactured in commercial quantities while adhering to all regulatory and
other
requirements, all at an acceptable cost. We may not be able to enter into future
third-party contract manufacturing agreements on acceptable terms, if at all.
We
expect
to continue to rely on contract manufacturers and other third parties to produce
sufficient quantities of our drug candidates for use in our clinical trials.
See
“Business - Business Overview - Supply and Manufacturing” below. We believe that
our existing manufacturing arrangements with these parties will be adequate
to
satisfy our current clinical supply needs for XTL-6865 and our planned clinical
supply needs for XTL-2125. Future supply of the HepeX-B clinical material will
be manufactured by a contract manufacturer to be selected by our partner Cubist
Pharmaceuticals Inc. If our contract manufacturers or other third parties fail
to deliver our product candidates for clinical use on a timely basis, with
sufficient quality, and at commercially reasonable prices, and we fail to find
replacement manufacturers, we may be required to delay or suspend clinical
trials or otherwise discontinue development and production of our drug
candidates.
Our
contract manufacturers are required to produce our drug candidates in strict
compliance with current good manufacturing practices, or cGMP, in order to
meet
acceptable standards for our clinical trials. If such standards change, the
ability of contract manufacturers to produce our drug candidates on the schedule
we require for our clinical trials may be affected. In addition, contract
manufacturers may not perform their obligations under their agreements with
us
or may discontinue their business before the time required by us to successfully
produce and market our drug candidates. Any difficulties or delays in our
contractors’ manufacturing and supply of drug candidates could increase our
costs, cause us to lose revenue or make us postpone or cancel clinical trials.
In
addition, our contract manufacturers will be subject to ongoing periodic,
unannounced inspections by the FDA and corresponding foreign governmental
agencies to ensure strict compliance with, among other things, current good
manufacturing practices, in addition to other governmental regulations and
corresponding foreign standards. We will not have control over, other than
by
contract, third-party manufacturers’ compliance with these regulations and
standards. No assurance can be given that our third-party manufacturers will
comply with these regulations or other regulatory requirements now or in the
future.
In
the
event that we are unable to obtain or retain third-party manufacturers, we
will
not be able to commercialize our products as planned. If third-party
manufacturers fail to deliver the required quantities of our products on a
timely basis and at commercially reasonable prices, our ability to develop
and
deliver products on a timely and competitive basis may be adversely impacted
and
our business, financial condition or results of operations will be materially
harmed.
If
our competitors develop and market products that are less expensive, more
effective or safer than our products, our commercial opportunities may be
reduced or eliminated.
The
pharmaceutical industry is highly competitive. Our commercial opportunities
may
be reduced or eliminated if our competitors develop and market products that
are
less expensive, more effective or safer than our products. Other companies
have
drug candidates in various stages of pre-clinical or clinical development to
treat diseases for which we are also seeking to discover and develop drug
candidates. For a discussion of these competitors and their drug candidates,
see
“Business - Business Overview - Competition” below. Some of these potential
competing drugs are further advanced in development than our drug candidates
and
may be commercialized earlier. Even if we are successful in developing safe,
effective drugs, our products may not compete successfully with products
produced by our competitors, who may be able to more effectively market their
drugs.
Our
competitors include pharmaceutical companies and biotechnology companies, as
well as universities and public and private research institutions. In addition,
companies that are active in different but related fields represent substantial
competition for us. Many of our competitors have significantly greater capital
resources, larger research and development staffs and facilities and greater
experience in drug development, regulation, manufacturing and marketing than
we
do. These organizations also compete with us to recruit qualified personnel,
attract partners for joint ventures or other collaborations, and license
technologies that are competitive with ours. As a result, our competitors may
be
able to more easily develop products that could render our technologies or
our
drug candidates obsolete or noncompetitive.
If
we lose our key personnel or are unable to attract and retain additional
personnel, our business could be harmed.
As
of
March 31, 2006, we had 42 full-time employees. To successfully develop our
drug
candidates and technologies, we must be able to attract and retain highly
skilled personnel. The retention of their services cannot be guaranteed. In
particular, if we lose the services of Michael S. Weiss, our Chairman, or Ron
Bentsur, our Chief Executive Officer, our ability to continue to execute on
our
business plan could be materially impaired. Our agreement with Mr. Weiss
provides that he may terminate his agreement with us upon 30 days’ prior written
notice if he is not re-elected as Chairman of our Board, his fees for service
as
Chairman are reduced by more than 10%, we breach any material term of his
agreement, or there is a change of control or reorganization of our company.
Our
agreement with Mr. Bentsur provides that he may terminate his agreement with
us
upon 30 days’ prior written notice if he is no longer the highest ranking member
of our company’s management team, his annual base salary is reduced by more than
10% (except where we have made similar deductions in the base salary of senior
management throughout our company), we breach any material term of his
agreement, or there is a change of control or reorganization of our company.
We
do not maintain a key man life insurance policy covering either Mr. Weiss or
Mr.
Bentsur.
Any
acquisitions we make may dilute your equity or require a significant amount
of
our available cash and may not be scientifically or commercially successful.
As
part
of our business strategy, we may effect acquisitions to obtain additional
businesses, products, technologies, capabilities and personnel. If we make
one
or more significant acquisitions in which the consideration includes our
ordinary shares or other securities, your equity in us may be significantly
diluted. If we make one or more significant acquisitions in which the
consideration includes cash, we may be required to use a substantial portion
of
our available cash.
Acquisitions
involve a number of operational risks, including:
|
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difficulty
and expense of assimilating the operations, technology and personnel
of
the acquired business;
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our
inability to retain the management, key personnel and other employees
of
the acquired business;
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our
inability to maintain the acquired company’s relationship with key third
parties, such as alliance partners;
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exposure
to legal claims for activities of the acquired business prior to
the
acquisition;
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the
diversion of our management’s attention from our core business; and
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the
potential impairment of substantial goodwill and write-off of in-process
research and development costs, adversely affecting our reported
results
of operations.
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If
any of
these risks occur, it could have an adverse effect on both the business we
acquire and our existing operations.
We
face product liability risks and may not be able to obtain adequate insurance.
The
use
of our drug candidates and technologies in clinical trials, and the sale of
any
approved products, exposes us to liability claims. Although we are not aware
of
any historical or anticipated product liability claims against us, if we cannot
successfully defend ourselves against product liability claims, we may incur
substantial liabilities or be required to cease clinical trials of our drug
candidates and technologies or limit commercialization of any approved products.
We
believe that we have obtained sufficient product liability insurance coverage
for our clinical trials. We intend to expand our insurance coverage to include
the commercial sale of any approved products if marketing approval is obtained;
however, insurance coverage is becoming increasingly expensive. We may not
be
able to maintain insurance coverage at a reasonable cost. We may not be able
to
obtain additional insurance coverage that will be adequate to cover product
liability risks that may arise. Regardless of merit or eventual outcome, product
liability claims may result in:
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decreased
demand for a product;
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injury
to our reputation;
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inability
to continue to develop a drug candidate or technology;
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withdrawal
of clinical trial volunteers; and
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loss
of revenues.
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Consequently,
a product liability claim or product recall may result in material
losses.
Risks
Related to Our Financial Condition
If
we are unable to obtain additional funds on terms favorable to us, or at all,
we
may not be able to continue our operations.
We
expect
to use, rather than generate, funds from operations for the foreseeable future.
We currently have an average projected burn rate of approximately $1.1 million
per month in 2006. Based on our current business plan, with the proceeds of
our
recent private placement that closed in March 2006, we believe we have
sufficient resources to fund our operations for approximately
the next 24 months; however, the actual amount of funds that we will need
will be determined by many factors, some of which are beyond our control. These
factors include:
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the
progress of our development activities;
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the
progress of our research activities;
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the
number and scope of our development programs;
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our
ability to establish and maintain current and new licensing or acquisition
arrangements;
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our
ability to achieve our milestones under our licensing arrangements;
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the
costs involved in enforcing patent claims and other intellectual
property
rights; and
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the
costs and timing of regulatory approvals.
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We
may
seek additional capital through a combination of public and private equity
offerings, debt financings and collaborative, strategic alliance and licensing
arrangements. We have
made
no determination at this time as to the amount, method or timing of any such
financing. Such
additional financing may not be available when we need it.
If we
are unable to obtain additional funds on terms favorable to us or at all, we
may
be required to cease or reduce our operating activities or sell or license
to
third parties some or all of our technology. If we raise additional funds by
selling ordinary shares or other securities, the ownership interests of our
shareholders will be diluted. If we need to raise additional funds through
the
sale or license of our drug candidates or technology, we may be unable to do
so
on terms favorable to us.
We
may be exposed to a significant tax assessment in Israel, which, if payable,
could adversely affect our available resources.
In
2005,
we received an assessment from the Israeli tax authorities of approximately
$730,000 (including fines and interest expenses) related to withholding taxes
for taxable employee benefits and taxable income in Israel paid to foreign
companies during the periods of 2001-2004. We have recorded an accrual which
we
believe reflects the probable liability associated with this assessment. There
can be no assurance that this accrual will be sufficient to cover the actual
assessment, if any.
We
may become subject to taxation in the United States, which could significantly
increase our tax liability in the United States for which we could not apply
the
net losses accumulated in Israel.
The
residency of the Chairman of our Board of Directors and our Chief Executive
Officer in the United States, as well as other less significant contacts we
have
with the U.S. could lead to a determination by the U.S. Internal Revenue Service
that we have a "permanent establishment" in the U.S. beginning in 2005. As
a
result, any income attributable to such permanent establishment in the U.S.
could be subject to U.S. corporate tax. If this is the case, we may not be
able
to utilize any of the accumulated loss carryforwards shown on our balance sheet
at December 31, 2005, to offset any such tax liability since they were all
accumulated under Israeli tax laws. U.S. corporate tax rates are higher than
those to which we are subject in the State of Israel, and if we are subject
to
U.S. corporate tax, it would have a material adverse effect on our results
of
operations.
Risks
Related to Our Intellectual Property
If
we are unable to adequately protect our intellectual property, third parties
may
be able to use our technology, which could adversely affect our ability to
compete in the market.
Our
commercial success will depend in part on our ability and the ability of our
licensors to obtain and maintain patent protection on our drug products and
technologies and successfully defend these patents and technologies against
third-party challenges. As part of our business strategy, our policy is to
actively file patent applications in the U.S. and internationally to cover
methods of use, new chemical compounds, pharmaceutical compositions and dosing
of the compounds and composition and improvements in each of these. See
“Business - Business Overview - Intellectual Property and Patents” below
regarding our patent position with regard to our product
candidates.
The
patent positions of pharmaceutical and biotechnology companies can be highly
uncertain and involve complex legal and factual questions. No consistent policy
regarding the breadth of claims allowed in biotechnology patents has emerged
to
date. Accordingly, the patents we use may not be sufficiently broad to prevent
others from practicing our technologies or from developing competing products.
Furthermore, others may independently develop similar or alternative
technologies or design around our patented technologies. The patents we use
may
be challenged or invalidated or may fail to provide us with any competitive
advantage. Moreover, in certain parts of the world, such as in China, western
companies are adversely affected by poor enforcement of intellectual property
rights. See “Business - Business Overview - License Agreements and
Collaborations” below regarding our license of Ab65, a component of
XTL-6865.
Generally,
patent applications in the U.S. are maintained in secrecy for a period of
18 months or more. Since publication of discoveries in the scientific or
patent literature often lag behind actual discoveries, we are not certain that
we were the first to make the inventions covered by each of our pending patent
applications or that we were the first to file those patent applications. We
cannot predict the breadth of claims allowed in biotechnology and pharmaceutical
patents, or their enforceability. Third parties or competitors may challenge
or
circumvent our patents or patent applications, if issued. If our competitors
prepare and file patent applications in the United States that claim compounds
or technology also claimed by us, we may choose to participate in interference
proceedings declared by the United States Patent and Trademark Office to
determine priority of invention, which could result in substantial cost, even
if
the eventual outcome is favorable to us. While we have the right to defend
patent rights related to the licensed drug candidates and technologies, we
are
not obligated to do so. In the event that we decide to defend our licensed
patent rights, we will be obligated to cover all of the expenses associated
with that effort. Because of the extensive time required for development,
testing and regulatory review of a potential product, it is possible that before
we commercialize any of our products, any related patent may expire or remain
in
existence for only a short period following commercialization, thus reducing
any
advantage of the patent.
Moreover,
we rely on trade secrets to protect technology where we believe patent
protection is not appropriate or obtainable. Trade secrets are difficult to
protect. While we require our employees, collaborators and consultants to enter
into confidentiality agreements, this may not be sufficient to adequately
protect our trade secrets or other proprietary information. In addition, we
share ownership and publication rights to data relating to some of our drug
candidates and technologies with our research collaborators and scientific
advisors. If we cannot maintain the confidentiality of this information, our
ability to receive patent protection or protect our proprietary information
will
be at risk.
Specifically,
we intend to apply for patent protection for each new monoclonal antibody
produced. Such patents may include claims relating to novel human monoclonal
antibodies directed at targets for which other human monoclonal antibodies
already exist, or at targets which are protected by patents or patent
applications filed by third parties. No assurance can be given that any such
patent application by a third-party will not have priority over patent
applications filed by us.
Several
groups are attempting to produce and patent a chimeric mouse with human tissue.
To the extent any patents issued to other parties claiming, in general,
mouse-human chimeras, the risk increases that the potential products and
processes of our or our future strategic partners may give rise to claims of
patent infringement.
We
plan
to use the recombinant production of antibodies in Chinese Hamster Ovary cells,
or CHO cells, in the development and production of some of our products. Patents
relating to this method of antibody production are owned by third-parties.
We
are also aware that third parties have patent protection covering hepatitis
C
antigens and antibodies, which will be needed in order to commercialize
XTL-6865. If we or our collaborative partners are unable to license such patent
rights on commercially acceptable terms, the ability to develop, manufacture
and
sell these products could be impaired. Further, royalties payable to third
parties may reduce the payments we will receive from our licensees or
development partners.
In
addition to patent protection, we may utilize orphan drug regulations to provide
market exclusivity for certain of our drug candidates. The orphan drug
regulations of the FDA provide incentives to pharmaceutical and biotechnology
companies to develop and manufacture drugs for the treatment of rare diseases,
currently defined as diseases that exist in fewer than 200,000 individuals
in
the United States, or, diseases that affect more than 200,000 individuals in
the
United States but that the sponsor does not realistically anticipate will
generate a net profit. Under these provisions, a manufacturer of a designated
orphan drug can seek tax benefits, and the holder of the first FDA approval
of a
designated orphan product will be granted a seven-year period of marketing
exclusivity for such FDA-approved orphan product. We believe that certain of
the
indications for our drug candidates will be eligible for orphan drug
designation. However, we cannot guarantee that any drug candidates will qualify,
and, if any do qualify, that we will be the holder of the first FDA approval
of
such qualifying drug candidates.
Litigation
or third-party claims of intellectual property infringement could require us
to
spend substantial time and money defending such claims and adversely affect
our
ability to develop and commercialize our products.
Third
parties may assert that we are using their proprietary technology without
authorization. In addition, third parties may have or obtain patents in the
future and claim that our products infringe their patents. If we are required
to
defend against patent suits brought by third parties, or if we sue third parties
to protect our patent rights, we may be required to pay substantial litigation
costs, and our management’s attention may be diverted from operating our
business. In addition, any legal action against our licensors or us that seeks
damages or an injunction of our commercial activities relating to the affected
products could subject us to monetary liability and require our licensors or
us
to obtain a license to continue to use the affected technologies. We cannot
predict whether our licensors or we would prevail in any of these types of
actions or that any required license would be made available on commercially
acceptable terms, if at all.
In
addition, there can be no assurance that our patents or patent applications
or
those licensed to us will not become involved in opposition or revocation
proceedings instituted by third parties. If such proceedings were initiated
against one or more of our patents, or those licensed to us, the defense of
such
rights could involve substantial costs and the outcome could not be
predicted.
Competitors
or potential competitors may have filed applications for, may have been granted
patents for, or may obtain additional patents and proprietary rights that may
relate to compounds or technologies competitive with ours. If patents are
granted to other parties that contain claims having a scope that is interpreted
to cover any of our products (including the manufacture thereof), there can
be
no assurance that we will be able to obtain licenses to such patents at
reasonable cost, if at all, or be able to develop or obtain alternative
technology.
Risks
Related to Our Ordinary Shares and ADRs
Our
ADRs are traded in small volumes, limiting your ability to sell the ADRs you
will receive that represent ordinary shares at a desirable price, if at
all.
The
trading volume of our ADRs has traditionally been very low. Even if the trading
volume of our ADRs increases, we can give no assurance that it will be
maintained or will result in a desirable stock price. As a result of this low
trading volume, it may be difficult to identify buyers to whom you can sell
your
ADRs and you may be unable to sell your ADRs at an established market price,
at
a price that is favorable to you, or at all. A low volume market also limits
your ability to sell large blocks of our ADRs at a desirable or stable price
at
any one time. You should be prepared to own our ordinary shares and ADRs
indefinitely.
Sales
of substantial amounts of our ADRs in the public market could harm the market
price of our ADRs.
We
cannot
predict the effect, if any, that future sales of our ADRs in the public market,
or the availability of our ADRs for sale in the market, will have on the market
price of our ADRs. We, therefore, can give no assurance that sales of
substantial amounts of our ADRs in the public market, or the potential for
large
amounts of sales in the market, whether by investors in the recent private
placement, under any registration statement or otherwise, would not cause the
price of our ADRs to decline considerably or impair our future ability to raise
capital through sales of our ADRs.
Our
stock price can be volatile, which increases the risk of litigation and may
result in a significant decline in the value of your investment.
The
trading price of the ADRs representing our ordinary shares is likely to be
highly volatile and subject to wide fluctuations in price in response to various
factors, many of which are beyond our control. These factors include:
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developments
concerning our drug candidates;
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announcements
of technological innovations by us or our competitors;
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introductions
or announcements of new products by us or our competitors;
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announcements
by us of significant acquisitions, strategic partnerships, joint
ventures
or capital commitments;
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changes
in financial estimates by securities analysts;
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actual
or anticipated variations in interim operating results;
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expiration
or termination of licenses, research contracts or other collaboration
agreements;
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conditions
or trends in the regulatory climate and the biotechnology and
pharmaceutical industries;
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changes
in the market valuations of similar companies; and
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additions
or departures of key personnel.
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In
addition, equity markets in general, and the market
for biotechnology and life sciences companies in particular, have experienced
extreme price and volume fluctuations that have often been unrelated or
disproportionate to the operating performance of companies traded in those
markets. These broad market and industry factors may materially affect the
market price of our ordinary shares, regardless of our development and operating
performance. In the past, following periods of volatility in the market price
of
a company’s securities, securities class-action litigation has often been
instituted against that company. Such litigation, if instituted against us,
could cause us to incur substantial costs to defend such claims and divert
management’s attention and resources even if we prevail in the litigation, all
of which could seriously harm our business.
Future
issuances of our ordinary shares could depress the market for our ordinary
shares and ADRs.
Future
issuances of a substantial number of our ordinary shares, or the perception
by
the market that those issuances could occur, could cause the market price of
our
ordinary shares or ADRs to decline or could make it more difficult for us to
raise funds through the sale of equity in the future.
If
we
make one or more significant acquisitions in which the consideration includes
ordinary shares or other securities, your equity in us may be significantly
diluted. Pursuant to a license agreement with VivoQuest, Inc., or VivoQuest,
a
privately held biotechnology company based in the U.S., we licensed (in all
fields of use) certain intellectual property and technology related to
VivoQuest’s HCV program, and we may elect to issue up to an additional $34.6
million in ordinary shares in lieu of cash to VivoQuest upon achievement of
certain milestones. In the future, we may enter into additional arrangements
with other third-parties permitting us to issue ordinary shares in lieu of
certain cash payments such as milestones.
Our
ordinary shares and ADRs trade on more than one market, and this may result
in
price variations.
Our
ordinary shares are traded on the London Stock Exchange and the Tel Aviv Stock
Exchange and ADRs representing our ordinary shares are quoted on the Nasdaq
National Market. Trading in our securities on these markets are made in
different currencies and at different times, including as a result of different
time zones, different trading days and different public holidays in the United
States, Israel and the United Kingdom. Consequently, the effective trading
prices of our shares on these three markets may differ. Any decrease in the
trading price of our shares on one of these markets could cause a decrease
in
the trading price of our shares on the other market.
Holders
of our ordinary shares who are United States residents may be required to pay
additional income taxes.
There
is
a risk that we will be classified as a Passive Foreign Investment Company,
or
PFIC, for certain tax years. If we are classified as a PFIC, a U.S. holder
of
our ordinary shares or ADRs representing our ordinary shares will be subject
to
special federal income tax rules that determine the amount of federal income
tax
imposed on income derived with respect to the PFIC shares. We will be a PFIC
if
either 75% or more of our gross income in a tax year is passive income or the
average percentage of our assets (by value) that produce or are held for the
production of passive income is at least 50%. The risk that we will be
classified as a PFIC arises because under applicable rules issued by the U.S.
Internal Revenue Service, or the IRS, cash balances, even if held as working
capital, are considered to be assets that produce passive income. Therefore,
any
determination of PFIC status will depend upon the sources of our income and
the
relative values of passive and non- passive assets, including goodwill. A
determination as to a corporation’s status as a PFIC must be made annually. We
believe that we were a PFIC for the taxable year ended December 31, 2003. We
believe that we were likely not a PFIC for the taxable years ended December
31,
2004 and 2005. Although such a determination is fundamentally factual in nature
and generally cannot be made until the close of the applicable taxable year,
based on our current operations, we believe that there is a significant
likelihood that we will be classified as a PFIC in the 2006 taxable year and
possibly in subsequent years.
If
we are
classified as a PFIC at any time during the U.S. holder’s holding period for our
stock, the federal income tax imposed on a U.S. holder with respect to income
derived from our stock will be determined under a special regime, which applies
upon (a) the receipt of any “excess distribution” from us (generally,
distributions in any year that are greater than 125% of the average annual
distributions received by such U.S. holder in the three preceding years or
its
holding period, if shorter) and (b) the sale or disposition of our stock.
Under
this special regime, the excess distribution or realized gain is treated
as
ordinary income. The federal income tax on such ordinary income is determined
under the following steps: (i) the amount of the excess distribution or gain
is
allocated ratably over the U.S. holder's holding period; (ii) tax is determined
for amounts allocated to the first such year in which we qualified as a PFIC
and
all subsequent years (except the year in which the excess distribution or
the
sale occurred) by applying the highest applicable tax rate in effect in the
year
to which the income was allocated; (iii) an interest charge is added to this
tax
calculated by applying the underpayment interest rate to the tax for each
year
determined under the preceding sentence for the period from the due date
of the
income tax return for such year to the due date of the return for the year
in
which in which the excess distribution or the disposition occurred; and (iv)
amounts allocated to a year prior to the first year in the U.S. holder’s holding
period in which we were a PFIC or to the year in which the excess distribution
or the disposition occurred are taxed as ordinary income and no interest
charge
applies.
A
U.S.
holder may generally avoid this regime by electing to treat its PFIC shares
as a
“qualified electing fund.” If a U.S. holder elects to treat PFIC shares as a
qualified electing fund, the U.S. holder must include annually in gross income
(for each year in which PFIC status is met) his pro rata share of the PFIC’s
ordinary earnings and net capital gains, whether or not such amounts are
actually distributed to the U.S. holder. Since fiscal 2005, we have complied
with the record-keeping and reporting requirements that are a prerequisite
to
making a “qualified electing fund” election. While we plan to continue to comply
with such requirements, if, in the future, meeting those record-keeping and
reporting requirements becomes onerous, we may decide, in our sole discretion,
that such compliance is impractical and will so notify U.S. holders.
In
view
of the complexity of the issues regarding our treatment as a PFIC, U.S.
shareholders are urged to consult their own tax advisors for guidance as to
our
status as a PFIC.
For
further discussion of tax consequences if we are a PFIC, see “Taxation - United
States Federal Income Tax Considerations - Tax Consequences If We Are A Passive
Foreign Investment Company” below.
Provisions
of Israeli corporate law may delay, prevent or affect a potential acquisition
of
all or a significant portion of our shares or assets and therefore depress
the
price of our ordinary shares.
Israeli
corporate law regulates acquisitions of shares through tender offers. It
requires special approvals for transactions involving significant shareholders
and regulates other matters that may be relevant to these types of transactions.
The provisions of Israeli law may delay or prevent an acquisition, or make
it
less desirable to a potential acquirer and therefore depress the price of our
shares. Further, Israeli tax considerations may make potential transactions
undesirable to us or to some of our shareholders.
Israeli
corporate law provides that an acquisition of shares in a public company must
be
made by means of a tender offer if, as a result of such acquisition, the
purchaser would become shareholder with over 25% of the voting rights in the
company. This rule does not apply if there is already another shareholder of
the
company with 25% or more of the voting rights. Similarly, Israeli corporate
law
provides that an acquisition of shares in a public company must be made by
means
of a tender offer if, as a result of the acquisition, the purchaser's
shareholdings would entitle the purchaser to over 45% of the voting rights
in
the company, unless there is a shareholder with 50% or more of the voting rights
in the company. These rules do not apply if the acquisition is made by way
of a
merger. Regulations promulgated under Israeli corporate law provide that these
tender offer requirements do not apply to companies whose shares are listed
for
trading outside of Israel if, according to the law in the country in which
the
shares are traded, including the rules and regulations of the stock exchange
or
which the shares are traded, either:
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there
is a limitation on acquisition of any level of control of the company;
or
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the
acquisition of any level of control requires the purchaser to do
so by
means of a tender offer to the
public.
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Finally,
in general, Israeli tax law treats specified acquisitions less favorably than
does U.S. tax law. See "Taxation -Israeli Tax Considerations" below.
Our
ADR holders are not shareholders and do not have shareholder
rights
The
Bank
of New York, as depositary, executes and delivers our American Depositary
Receipts, or ADRs, on our behalf. Each ADR is a certificate evidencing a
specific number of American Depositary Shares, also referred to as ADSs. Our
ADR
holders will not be treated as shareholders and do not have the rights of
shareholders. The depositary will be the holder of the shares underlying our
ADRs. Holders of our ADRs will have ADR holder rights. A deposit agreement
among
us, the depositary and our ADR holders, and the beneficial owners of ADRs,
sets
out ADR holder rights as well as the rights and obligations of the depositary.
New York law governs the deposit agreement and the ADRs. For a description
of
ADR holder rights, see “Description of American Depositary Shares.” Our
shareholders have shareholder rights. Israeli law and our Articles of
Association govern shareholder rights. For a description of our shareholders’
rights, see “Share Capital - Articles of Association - Rights Attached to
Ordinary Shares.” Our ADR holders do not have the same voting rights as our
shareholders. Shareholders are entitled to our notices of general meetings
and
to attend and vote at our general meetings of shareholders. At a general
meeting, every shareholder present (in person or by proxy, attorney or
representative) and entitled to vote has one vote on a show of hands. Every
shareholder present (in person or by proxy, attorney or representative) and
entitled to vote has one vote per fully paid ordinary share on a poll. This
is
subject to any other rights or restrictions which may be attached to any shares.
Our ADR holders may instruct the depositary to vote the ordinary shares
underlying their ADRs, but only if we ask the depositary to ask for their
instructions. If we do not ask the depositary to ask for the instructions,
our
ADR holders are not entitled to receive our notices of general meeting or
instruct the depositary how to vote. Our ADR holders will not be entitled to
attend and vote at a general meeting unless they withdraw the ordinary shares.
However, our ADR holders may not know about the meeting enough in advance to
withdraw the shares. If we ask for our ADR holders’ instructions, the depositary
will notify our ADR holders of the upcoming vote and arrange to deliver our
voting materials and form of notice to them. The depositary will try, as far
as
practical, subject to the provisions of the deposit agreement, to vote the
shares as our ADR holders instruct. The depositary will not vote or attempt
to
exercise the right to vote other than in accordance with the instructions of
the
ADR holders. We cannot assure our ADR holders that they will receive the voting
materials in time to ensure that they can instruct the depositary to vote their
shares. In addition, there may be other circumstances in which our ADR holders
may not be able to exercise voting rights.
Our
ADR
holders do not have the same rights to receive dividends or other distributions
as our shareholders. Subject to any special rights or restrictions attached
to a
share, the directors may determine that a dividend will be payable on a share
and fix the amount, the time for payment and the method for payment (although
we
have never declared or paid any cash dividends on our ordinary stock and we
do
not anticipate paying any cash dividends in the foreseeable future). Dividends
may be paid on shares of one class but not another and at different rates for
different classes. Dividends and other distributions payable to our shareholders
with respect to our ordinary shares generally will be payable directly to them.
Any dividends or distributions payable with respect to ordinary shares will
be
paid to the depositary, which has agreed to pay to our ADR holders the cash
dividends or other distributions it or the custodian receives on shares or
other
deposited securities, after deducting its fees and expenses. Our ADR holders
will receive these distributions in proportion to the number of shares their
ADSs represent. In addition, there may be certain circumstances in which the
depositary may not pay to our ADR holders amounts distributed by us as a
dividend or distribution. See the risk factor “- There are circumstances where
it may be unlawful or impractical to make distributions to the holders of our
ADRs” below.
There
are circumstances where it may be unlawful or impractical to make distributions
to the holders of our ADRs.
The
deposit agreement with the depositary allows the depositary to distribute the
foreign currency only to those ADR holders to whom it is possible to do so.
If a
distribution is payable by us in New Israeli Shekels or Pounds Sterling, the
depositary will hold the foreign currency it cannot convert for the account
of
the ADR holders who have not been paid. It will not invest the foreign currency
and it will not be liable for any interest. If the exchange rates fluctuate
during a time when the depositary cannot convert the foreign currency, our
ADR
holders may lose some of the value of the distribution.
The
depositary is not responsible if it decides that it is unlawful or impractical
to make a distribution available to any ADR holders. This means that our ADR
holders may not receive the distributions we make on our shares or any value
for
them if it is illegal or impractical for us to make them available to
them.
Risks
Relating to Operations in Israel
Conditions
in the Middle East and in Israel may harm our
operations.
Certain
of our research and development facilities and some of our suppliers are located
in Israel. Political, economic and military conditions in Israel directly affect
our operations. Since the establishment of the State of Israel in 1948, a number
of armed conflicts have taken place between Israel and its Arab neighbors,
as
well as incidents of civil unrest, military conflicts and terrorist actions.
There has been a significant increase in violence since September 2000, which
has continued with varying levels of severity through to the present. This
state
of hostility has caused security and economic problems for Israel. To date,
we
do not believe that the political and security situation has had a material
adverse impact on our business, but we cannot give you any assurance that this
will continue to be the case. Any hostilities involving Israel or the
interruption or curtailment of trade between Israel and its present trading
partners could adversely affect our operations and could make it more difficult
for us to raise capital.
Our
commercial insurance does not cover losses that may occur as a result of events
associated with the security situation in the Middle East. Although the Israeli
government currently covers the reinstatement value of direct damages that
are
caused by terrorist attacks or acts of war, we cannot assure you that this
government coverage will be maintained. Any losses or damages incurred by us
could have a material adverse effect on our business. Any armed conflicts or
political instability in the region would likely negatively affect business
conditions and could harm our results of operations.
Further,
in the past, the State of Israel and Israeli companies have been subjected
to an
economic boycott. Several countries still restrict business with the State
of
Israel and with Israeli companies. These restrictive laws and policies may
have
an adverse impact on our operating results, financial condition or the expansion
of our business.
Our
results of operations may be adversely affected by inflation and foreign
currency fluctuations.
We
generate all of our revenues and hold most of our cash, cash equivalents, bank
deposits and marketable securities in U.S. dollars. While a substantial amount
of our operating expenses are in U.S. dollars, we incur a portion of our
expenses in New Israeli Shekels (approximately 20% in 2005). In addition, we
also pay for some of our services and supplies in the local currencies of our
suppliers. As a result, we are exposed to the risk that the U.S. dollar will
be
devalued against the New Israeli Shekel or other currencies, and as result
our
financial results could be harmed if we are unable to guard against currency
fluctuations in Israel or other countries in which services and supplies are
obtained in the future. Accordingly, we may in the future enter into currency
hedging transactions to decrease the risk of financial exposure from
fluctuations in the exchange rates of currencies. These measures, however,
may
not adequately protect us from the adverse effects of inflation in Israel.
In
addition, we are exposed to the risk that the rate of inflation in Israel will
exceed the rate of devaluation of the New Israeli Shekel in relation to the
dollar or that the timing of any devaluation may lag behind inflation in Israel.
The
Office of the Chief Scientist may refuse to approve the manufacture of our
products outside the State of Israel.
We
have
in the past participated in programs offered by the Office of the Chief
Scientist under the Industry, Trade and Labor Ministry of Israel that supports
research and development activities. Through December 31, 2005, we have received
$7.3 million in grants from the Office of the Chief Scientist for several
projects, most of which are currently under development. Israeli law requires
that the manufacture of products developed with government grants be carried
out
in Israel, unless the Office of the Chief Scientist provides a special approval
to the contrary. This approval, if provided, is generally conditioned on an
increase in the total amount to be repaid to the Office of the Chief Scientist
to between 120% and 300% of the amount of funds granted. While we believe that
the Office of the Chief Scientist does not unreasonably withhold approval if
the
request is based upon commercially justified circumstances and any royalty
obligations to the Office of the Chief Scientist are sufficiently assured,
the
matter is solely within its discretion. We cannot be sure that such approval,
if
requested, would be granted upon terms satisfactory to us or granted at all.
Without such approval, we would be unable to manufacture any products developed
by this research outside of Israel, which may greatly restrict any potential
revenues from such products.
We
may not continue to be entitled to certain tax benefits from the Israeli
government.
We
are
entitled to receive certain tax benefits as a result of the Approved Enterprise
status of our existing facilities in Israel. The Law for the Encouragement
of
Capital Investment, 1959, as amended, provides that a proposed capital
investment in eligible facilities may, upon application to the Investment Center
of the Ministry of Industry and Trade of the State of Israel, permit a company
to recognize taxable income attributable to the Approved Enterprise subject
to
company tax at the maximum rate of 25% rather than the usual rate in 2006 of
31%. This usual rate is currently scheduled to decrease as follows: in 2007
-
29%, 2008 - 27%, 2009 - 26%, 2010 and after - 25%. For further discussion of
these tax benefits, see “Taxation - Israeli Tax Considerations” below. To date
we have not received any such tax benefits because we have not generated any
taxable income to date. To maintain our eligibility for these tax benefits,
we
must meet certain reporting requirements and certain conditions that we have
either obligated ourselves to meet or that are included in the Certificate
of
Approval from the Investment Center of the Ministry of Industry and Trade of
the
State of Israel. If we cease to become entitled to tax benefits, we may be
required to pay repay corporate tax at the normal rate on all or part of the
taxable income that we may generate from the eligible facilities in the future.
It
may be difficult to enforce a U.S. judgment against us, our officers or our
directors or to assert U.S. securities law claims in
Israel.
Service
of process upon us, since we are incorporated in Israel, and upon our directors
and officers and our Israeli auditors, some of whom reside outside the United
States, may be difficult to obtain within the United States. In addition,
because substantially all of our assets and some of our directors and officers
are located outside the United States, any judgment obtained in the United
States against us or any of our directors and officers may not be collectible
within the United States. There is a doubt as to the enforceability of civil
liabilities under the Securities Act or the Exchange Act pursuant to original
actions instituted in Israel. Subject to particular time limitations and
provided certain conditions are met, executory judgments of a United States
court for monetary damages in civil matters may be enforced by an Israeli court.
For
more
information regarding the enforceability of civil liabilities against us, our
directors and our executive officers, see “Description of Share Capital-
Memorandum and Articles of Association - Enforceability of Civil Liabilities”
below.
Except
for proceeds, if any, received in connection with the exercise of warrants,
we
will not receive any proceeds from the sale of ADRs by the Selling Shareholders.
Any proceeds received in connection with the exercise of warrants will be used
for general corporate purposes.
Ordinary
Shares
The
primary trading market for our ordinary shares, having a nominal value of NIS
0.02, is the London Stock Exchange, where our shares have been listed and traded
under the symbol “XTL” since our initial public offering in September of 2000.
As of July 12, 2005, our ordinary shares are also listed on the Tel Aviv Stock
Exchange under the symbol “XTL.” Since September 1, 2005, our ADRs have been
traded on the Nasdaq Stock Market under the symbol “XTLB,” with each ADR
representing ten ordinary shares.
The
following table sets forth, for the periods indicated, the high and low reported
sales prices of the ordinary shares on the London Stock Exchange. For
comparative purposes only, we have also provided such figures translated into
U.S. Dollars at an exchange rate of 1.742 U.S. Dollars per British Pound, as
reported by the Bank of Israel on March 31, 2006.
|
|
British
Pence (p)
|
U.S.
Dollar
|
|||||||||||
|
Last
Six Calendar Months
|
High
|
Low
|
High
|
Low
|
|||||||||
|
March
2006
|
44.00
|
34.25
|
0.77
|
0.60
|
|||||||||
|
February
2006
|
40.25
|
35.25
|
0.70
|
0.61
|
|||||||||
|
January
2006
|
45.00
|
40.25
|
0.78
|
0.70
|
|||||||||
|
December
2005
|
48.25
|
42.00
|
0.84
|
0.73
|
|||||||||
|
November
2005
|
53.00
|
44.75
|
0.92
|
0.78
|
|||||||||
|
October
2005
|
52.25
|
44.75
|
0.91
|
0.78
|
|||||||||
|
Financial
Quarters During the Past Two Full Fiscal Years
|
|||||||||||||
|
First
Quarter of 2006
|
45.00
|
34.25
|
0.78
|
0.60
|
|||||||||
|
Fourth
Quarter of 2005
|
53.00
|
42.00
|
0.92
|
0.73
|
|||||||||
|
Third
Quarter of 2005
|
61.75
|
38.00
|
1.08
|
0.66
|
|||||||||
|
Second
Quarter of 2005
|
40.50
|
36.00
|
0.71
|
0.63
|
|||||||||
|
First
Quarter of 2005
|
43.50
|
26.00
|
0.76
|
0.45
|
|||||||||
|
Fourth
Quarter of 2004
|
25.50
|
13.00
|
0.44
|
0.23
|
|||||||||
|
Third
Quarter of 2004
|
19.50
|
13.75
|
0.34
|
0.24
|
|||||||||
|
Second
Quarter of 2004
|
32.25
|
17.00
|
0.56
|
0.30
|
|||||||||
|
Last
Five Full Financial Years
|
|||||||||||||
|
2005
|
61.75
|
26.00
|
1.08
|
0.45
|
|||||||||
|
2004
|
32.25
|
13.00
|
0.56
|
0.23
|
|||||||||
|
2003
|
18.75
|
5.75
|
0.33
|
0.10
|
|||||||||
|
2002
|
64.00
|
11.50
|
1.11
|
0.20
|
|||||||||
|
2001
|
153.00
|
33.50
|
2.67
|
0.58
|
|||||||||
The
following table sets forth, for the periods indicated, the high and low sales
prices of the ordinary shares on the Tel
Aviv
Stock Exchange.
For
comparative purposes only, we have also provided such figures translated into
U.S. Dollars at an exchange rate of 4.665 New Israeli Shekel per U.S. Dollar,
as
reported by the Bank of Israel on March 31, 2006.
|
|
New
Israeli Shekel
|
U.S.
Dollar
|
|||||||||||
|
Last
Six Calendar Months
|
High
|
Low
|
High
|
Low
|
|||||||||
|
March
2006
|
3.61
|
2.86
|
0.77
|
0.61
|
|||||||||
|
February
2006
|
3.35
|
2.93
|
0.72
|
0.63
|
|||||||||
|
January
2006
|
3.66
|
3.21
|
0.78
|
0.69
|
|||||||||
|
December
2005
|
3.94
|
3.44
|
0.84
|
0.74
|
|||||||||
|
November
2005
|
4.31
|
3.69
|
0.92
|
0.79
|
|||||||||
|
October
2005
|
4.38
|
3.65
|
0.94
|
0.78
|
|||||||||
| Financial Quarters Since Listing | |||||||||||||
|
First
Quarter of 2006
|
3.66
|
2.86
|
0.78
|
0.61
|
|||||||||
|
Fourth
Quarter of 2005
|
4.38
|
3.44
|
0.94
|
0.74
|
|||||||||
American
Depositary Shares
The
following table presents, for the periods indicated, the high and low market
prices for our ADRs as reported on the Nasdaq Stock Market since September
1,
2005, the date on which our ADRs were initially quoted. Prior to the initial
quotation of our ADRs on the Nasdaq Stock Market on September 1, 2005, our
ADRs
were not traded in any organized market and were not liquid. For a description
of the rights of our ADRs, see “Description of American Depositary
Receipts.”
|
U.S.
Dollar
|
|||||||
|
Last
Six Calendar Months
|
High
|
Low
|
|||||
|
March 2006
|
7.95
|
6.13
|
|||||
|
February 2006
|
7.23
|
6.39
|
|||||
|
January 2006
|
8.12
|
6.90
|
|||||
|
December 2005
|
8.84
|
7.10
|
|||||
|
November 2005
|
9.08
|
7.86
|
|||||
|
October 2005
|
9.50
|
7.91
|
|||||
| Financial Quarters Since Listing | |||||||
|
First Quarter of 2006
|
8.12 | 6.13 | |||||
|
Fourth Quarter of 2005
|
9.50 | 7.10 | |||||
As
of
March 31, 2006, there were 572,551 ADRs outstanding in the United
States.
We
have
never declared or paid any cash dividends on our ordinary shares and do not
anticipate paying any such cash dividends in the foreseeable future. Any future
determination to pay dividends will be at the discretion of our board of
directors.
In
the
event that we decide to pay a cash dividend from income that is tax exempt
under
our approved enterprise status, we would be liable for corporate tax on the
amount distributed at the rate of up to 25%. See “Note 8 of our Consolidated
Financial Statements.” Cash dividends may be paid by an Israeli company only out
of retained earnings as calculated under Israeli law. We currently have no
retained earnings and do not expect to have any retained earnings in the
foreseeable future.
27
The
following table sets forth our capitalization as of December 31, 2005, as
adjusted to reflect the effect of our private placement of 46,666,670 ordinary
shares in the form of ADRs on March 22, 2006, and the receipt of the proceeds
therefrom, net of estimated fees.
You
should read this table in conjunction with “Selected Financial Data” and our
combined financial statements and related notes included elsewhere in this
prospectus.
|
(In
thousands, except per share amounts)
|
As
of
December
31, 2005
|
Private
Placement March 2006
|
As
Adjusted
|
|||||||
|
Cash,
cash equivalents, bank deposits and
marketable securities
|
$
|
13,360
|
$
|
24,400
|
$
|
37,760
|
||||
|
Shareholders’
equity:
|
||||||||||
|
Ordinary
shares of NIS 0.02 par value (authorized
300,000,000 as of December
31, 2005; issued and outstanding:
173,180,441 as of December
31, 2005; issued and outstanding as
adjusted for the private placement: 219,847,111)
|
864
|
200
|
1,064
|
|||||||
|
Additional
paid in capital
|
110,179
|
24,200
|
134,379
|
|||||||
|
Deficit
accumulated during development stage
|
(99,791
|
)
|
--
|
(99,791
|
)
|
|||||
|
Total
shareholders’ equity
|
11,252
|
24,400
|
35,652
|
|||||||
|
Total
capitalization
|
$
|
11,252
|
$
|
24,400
|
$
|
35,652
|
||||
The
table
below presents selected statement of operations and balance sheet data for
the
fiscal years ended and as of December 31, 2005, 2004, 2003, 2002 and 2001.
We
have derived the selected financial data for the fiscal years ended December
31,
2005, 2004, and 2003, and as of December 31, 2005 and 2004, from our audited
consolidated financial statements, included elsewhere in this prospectus and
prepared in accordance with U.S. GAAP. We have derived the selected financial
data for fiscal years ended December 31, 2002 and 2001 and as of December 31,
2003, 2002 and 2001, from audited financial statements not appearing in this
prospectus, which have been prepared in accordance with U.S. GAAP. You should
read the selected financial data in conjunction with “Management’s Discussion
and Analysis of Financial Condition and Results of Operations,” and our audited
consolidated financial statements include elsewhere in this
prospectus.
|
Year
Ended December 31,
|
||||||||||||||||
|
|
2005
|
2004
|
2003
|
2002
|
2001
|
|||||||||||
|
(In
thousands, except per share amounts)
|
||||||||||||||||
|
Statements
of Operations Data:
|
||||||||||||||||
|
Revenues
|
|
|
|
|
||||||||||||
|
Reimbursed
out of pocket expenses
|
$
|
2,743
|
$
|
3,269
|
$
|
--
|
$
|
--
|
$
|
--
|
||||||
|
License
|
454
|
185
|
--
|
--
|
--
|
|||||||||||
|
3,197
|
3,454
|
--
|
--
|
--
|
||||||||||||
|
Cost
of Revenues
|
|
|
|
|
||||||||||||
|
Reimbursed
out of pocket expenses
|
2,743
|
3,269
|
--
|
--
|
--
|
|||||||||||
|
License
|
54
|
32
|
--
|
--
|
--
|
|||||||||||
|
2,797
|
3,301
|
|
|
|
||||||||||||
|
Gross
Margin
|
400
|
153
|
--
|
--
|
--
|
|||||||||||
|
|
|
|
|
|
|
|||||||||||
|
Research
and development
|
|
|
|
|
|
|||||||||||
|
Research
and development costs
|
7,313
|
11,985
|
14,022
|
13,231
|
12,187
|
|||||||||||
|
Less
participations
|
--
|
--
|
3,229
|
75
|
1,133
|
|||||||||||
|
|
7,313
|
11,985
|
10,793
|
13,156
|
11,054
|
|||||||||||
|
In-process
research and development
|
1,783
|
--
|
--
|
--
|
--
|
|||||||||||
|
General
and administrative
|
5,457
|
4,134
|
3,105
|
3,638
|
3,001
|
|||||||||||
|
Business
development costs
|
227
|
810
|
664
|
916
|
1,067
|
|||||||||||
|
|
|
|
|
|||||||||||||
|
Operating
loss
|
(14,380
|
)
|
(16,776
|
)
|
(14,562
|
)
|
(17,710
|
)
|
(15,122
|
)
|
||||||
|
|
|
|
||||||||||||||
|
Other
income (expense)
|
|
|
|
|
||||||||||||
|
Financial
income, net
|
443
|
352
|
352
|
597
|
2,448
|
|||||||||||
|
Taxes
on income
|
(78
|
)
|
(49
|
)
|
(78
|
)
|
(27
|
)
|
--
|
|||||||
|
|
|
|
|
|
||||||||||||
|
Net
loss
|
$
|
(14,015
|
)
|
$
|
(16,473
|
)
|
$
|
(14,288
|
)
|
$
|
(17,140
|
)
|
$
|
(12,674
|
)
|
|
|
|
|
|
||||||||||||||
|
Net
loss per ordinary share
|
|
|
||||||||||||||
|
Basic
and diluted
|
$
|
(0.08
|
)
|
$
|
(0.12
|
)
|
$
|
(0.13
|
)
|
$
|
(0.15
|
)
|
$
|
(0.11
|
)
|
|
|
Weighted
average shares outstanding
|
170,123,003
|
134,731,766
|
111,712,916
|
111,149,292
|
110,941,014
|
|||||||||||
|
As
of December 31,
|
||||||||||||||||
|
|
2005
|
2004
|
2003
|
2002
|
2001
|
|||||||||||
|
|
(In
thousands, except per share amounts)
|
|||||||||||||||
|
Balance
Sheet Data:
|
||||||||||||||||
|
Cash,
cash equivalents, bank deposits and marketable
securities
|
$
|
13,360
|
$
|
22,924
|
$
|
22,262
|
$
|
35,706
|
$
|
52,188
|
||||||
|
Working
capital
|
11,385
|
20,240
|
19,967
|
33,396
|
50,433
|
|||||||||||
|
Total
assets
|
15,151
|
25,624
|
24,853
|
38,423
|
55,106
|
|||||||||||
|
Long-term
obligations
|
1,493
|
2,489
|
1,244
|
1,017
|
526
|
|||||||||||
|
Total
shareholders’ equity
|
11,252
|
19,602
|
20,608
|
34,830
|
51,953
|
|||||||||||
CONDITION
AND RESULTS OF OPERATIONS
The
following discussion and analysis contains forward-looking statements about
our
plans and expectations of what may happen in the future. Forward-looking
statements are based on a number of assumptions and estimates that are
inherently subject to significant risks and uncertainties, and our results
could
differ materially from the results anticipated by our forward-looking statements
as a result of many known or unknown factors, including, but not limited to,
those factors discussed in “Risk Factors.” See also the “Cautionary Note
Regarding Forward-Looking Statements” set forth above.
You
should read the following discussion and analysis in conjunction with our
audited consolidated financial statements, including the related notes, prepared
in accordance with U.S. GAAP for the years ended December 31, 2005, 2004, 2003,
2002 and 2001, and as of December 31, 2005, 2004, 2003, 2002 and 2001, contained
in “Selected Financial Data” above.
Executive
Summary
We
are a
biopharmaceutical company engaged in the acquisition, research, development
and
commercialization of pharmaceutical products for the treatment of infectious
diseases, particularly the treatment of hepatitis C. To date, we have not
received approval for the sale of any of our drug candidates in any market
and,
therefore, have not generated any commercial revenues from the sales of our
drug
candidates. We have received license and reimbursed out of pocket expense
revenue pursuant to our agreement with Cubist with respect to HepeX-B, although
HepeX-B has not yet been commercialized.
We
were
established as a corporation under the laws of the State of Israel in 1993,
and
commenced operations to use and commercialize technology developed at the
Weizmann Institute, in Rehovot, Israel. Since commencing operations, our
activities have been primarily devoted to developing our technologies and drug
candidates, acquiring pre-clinical and clinical-stage compounds, raising
capital, purchasing assets for our facilities, and recruiting personnel. We
are
a development stage company and have no product sales to date. Our major sources
of working capital have been proceeds from various private placements of equity
securities, option and warrant exercises, from our initial public offering
and
from our placing and open offer transaction.
We
have
incurred negative cash flow from operations each year since our inception and
we
anticipate incurring negative cash flows from operating activities for the
foreseeable future. We have spent, and expect to continue to spend, substantial
amounts in connection with implementing our business strategy, including our
planned product development efforts, our clinical trials and potential
in-licensing and acquisition opportunities.
Our
revenues currently consist of license fees and reimbursed out of pocket expenses
from Cubist, and may include certain additional payments contingent upon
achievement of regulatory milestones and royalties if our collaboration with
Cubist is successful. We recognize the license fee revenues from our agreement
with Cubist ratably over the expected term until regulatory approval is
obtained, with un-amortized amounts recorded as deferred revenues. We also
recognize revenue related to reimbursed out of pocket expenses at the time
that
that we provide development services to Cubist.
Our
cost
of revenues consist of costs associated with the Cubist program for HepeX-B
which consist primarily of salaries and related personnel costs, fees paid
to
consultants and other third-parties for clinical and laboratory development,
facilities-related and other expenses relating to the design, development,
testing, and enhancement of our product candidate out-licensed to Cubist. In
addition, we recognize license fee expenses associated with our agreement with
Yeda proportional to our license fee agreement with Cubist, with un-amortized
amounts recorded as deferred expenses.
Our
research and development costs consist primarily of salaries and related
personnel costs, fees paid to consultants and other third-parties for clinical
and laboratory development, facilities-related and other expenses relating
to
the design, development, testing, and enhancement of our product candidates.
We
expense our research and development costs as they are incurred.
Our
participations consist primarily of grants received from the Israeli government
in support of our research and development activities. These grants are
recognized as a reduction of expense as the related costs are incurred. See
“-
Research and Development, Patents and Licenses - Israeli Government Research
and
Development Grants” below.
Our
general and administrative expenses consist primarily of salaries and related
expenses for executive, finance and other administrative personnel, professional
fees, director fees and other corporate expenses, including investor relations,
and facilities related expenses. We expense our general and administrative
expenses as they are incurred.
Our
business development costs consist primarily of salaries and related expenses
for business development personnel, travel and professional fees. Our business
development activities are related to partnering activities for our drug
programs and for seeking new research and development collaborations. We expense
our business development expenses as they are incurred.
Our
results of operations include non-cash compensation expense as a result of
the
grants of stock options and warrants. Compensation expense for awards of options
granted to employees and directors represents the fair value of the award
recorded over the respective vesting periods of the individual stock options.
The expense is included in the respective categories of expense in the statement
of operations. We expect to incur significant non-cash compensation as a result
of adopting Statement of Financial Accounting Standards No. 123, “Share Based
Payment,” or FAS 123R, which we elected to adopt on January 1, 2005.
For
period presented prior to our adoption of FAS 123R, compensation expense for
fixed award options granted to employees and directors represented the intrinsic
value (the difference between the stock price of the common stock and the
exercise price of the options) of the options at the date of grant. For variable
awards, we considered the difference between the stock price at reporting date
and the exercise price, in the case where a measurement date has not been
reached. The compensation cost was recorded over the respective vesting periods
of the individual stock options and warrants. The expense was included in the
respective categories of expense in the statement of operations.
For
awards of options and warrants to consultants and other third-parties,
compensation expense is determined at the “measurement date.” The expense is
recognized over the vesting period for the award. Until the measurement date
is
reached, the total amount of compensation expense remains uncertain. We record
compensation expense based on the fair value of the award at the reporting
date.
These awards are then revalued, or the total compensation is recalculated based
on the then current fair value, at each subsequent reporting date.
Our
ongoing clinical trials will be lengthy and expensive. Even if these trials
show
that our drug candidates are effective in treating certain indications, there
is
no guarantee that we will be able to record commercial sales of any of our
product candidates in the near future. In addition, we expect losses to continue
as we continue to fund development of our drug candidates. As we continue our
development efforts, we may enter into additional third-party collaborative
agreements and may incur additional expenses, such as licensing fees and
milestone payments. As a result, our periodical results may fluctuate and a
period-by-period comparison of our operating results may not be a meaningful
indication of our future performance.
Results
of Operations
Years
Ended December 31, 2005 and 2004
Revenues.
Revenues
for the year ended December 31, 2005, decreased by $257,000 to $3,197,000,
as
compared to revenues of $3,454,000 for the year ended December 31, 2004. The
decrease in revenues for the year ended December 31, 2005, was due to a $526,000
decrease associated with the reimbursement for development expenses for HepeX-B
that were incurred pursuant to our licensing agreement with Cubist, partially
offset by an increase of $269,000 in licensing revenues pursuant to our
agreement with Cubist.
We
expect
our revenues to decrease significantly over the next year, pursuant to our
agreement with Cubist, under which we transferred full responsibility for
completing the development of HepeX-B to Cubist such that Cubist will be
responsible for completing the development and for registration and
commercialization of the product worldwide.
Cost
of Revenues.
Cost of
revenues for the year ended December 31, 2005, decreased by $504,000 to
$2,797,000, as compared to cost of revenues of $3,301,000, for the year ended
December 31, 2004. The decrease in cost of revenues was due to a $526,000
decrease in development expenses for HepeX-B that were incurred pursuant to
our
licensing agreement with Cubist, partially offset by a $22,000 increase in
licensing expense pursuant to our agreement with Yeda.
We
expect
our cost of revenues to decrease significantly over the next year, pursuant
to
our agreement with Cubist, as described above.
Research
and Development Costs.
Research and development costs decreased by $4,672,000 to $7,313,000 for the
year ended December 31, 2005, as compared to $11,985,000 for the year ended
December 31, 2004. The decrease in research and development costs was due
primarily to the absence of approximately $3,301,000 in expenses related to
the
development and clinical program of HepeX-B, due to the agreement with Cubist
and the subsequent inclusion of development costs related to HepeX-B in Cost
of
Revenues above and a decrease of approximately $2,746,000 in expenses related
to
the XTL-6865 development and clinical program. This decrease was partially
offset by an approximate $135,000 increase in expenses associated with XTL-2125
and an increase of $1,240,000 in expenses related to the inclusion of DOS from
September 2005 following the completion of the VivoQuest transaction. See
“Business - Material Contracts - VivoQuest, Inc.”
We
expect
our research and development costs to increase in 2006 due to expected research
and development expenditures associated with the planned clinical trial of
XTL-2125, the continuation of the XTL-6865 clinical trial, and the inclusion
of
a full year of our DOS program, offset by cost reductions associated with our
2005 restructuring.
Participations.
There
were no participations from the Office of the Chief Scientist for the years
ended December 31, 2005, and 2004, respectively. We ceased requesting grants
from the Office of the Chief Scientist in 2004 due to the potential contingent
liability associated with the transfer of manufacturing rights outside of
Israel.
In-Process
Research and Development.
For the
year ended December 31, 2005, we incurred a charge of $1,783,000 for the
estimate of the portion of the VivoQuest transaction purchase price allocated
to
in-process research and development.
General
and Administrative Expenses.
General
and administrative expenses increased by $1,323,000 to $5,457,000 for the year
ended December 31, 2005, as compared to expenses of $4,134,000 for the year
ended December 31, 2004. The increase in general and administrative expenses
was
due primarily to an increase in non-cash compensation costs of $2,641,000,
primarily related to the grant of options to certain of our directors, offset
by
a decrease in expenses following our 2005 restructuring.
Not
including non-cash compensation costs, we expect our general and administrative
costs to increase modestly in 2006 as the result of hiring our new Chief
Executive Officer and due to increased costs associated with complying with
U.S.
public company requirements.
Business
Development Costs.
Business development costs decreased by approximately $583,000 to $227,000
for
the year ended December 31, 2005, as compared to expenses of $810,000 for the
year ended December 31, 2004. The decrease in business developments costs was
due primarily to reduced compensation costs and reduced professional fees.
Financial
Income.
Financial income for the year ended December 31, 2005, increased by $91,000
to
$443,000, as compared to financial income of $352,000 for the year ended
December 31, 2004. The increase in financial income was due primarily to
increased interest income due to the general increase in short-term market
interest rates when compared to the comparable period last year.
Income
Taxes.
Income
tax expense increased by $29,000 to $78,000 for the year ended December 31,
2005, as compared to expenses of $49,000 for year ended December 31, 2004.
Our
income tax expense is attributable to taxable income from the continuing
operations of our subsidiary in the United States. This income is eliminated
upon consolidation of our financial statements.
Years
Ended December 31, 2004 and 2003
Revenues.
Revenues
for the year ended December 31, 2004, were $3,454,000, as compared to no
revenues for the year ended December 31, 2003. Revenues for the year ended
December 31, 2004, were due to $3,269,000 associated with reimbursement for
development expenses for HepeX-B that were incurred pursuant to our licensing
agreement with Cubist, as well as to $185,000 in licensing revenues pursuant
to
our agreement with Cubist.
Cost
of Revenues.
Cost of
revenues for the year ended December 31, 2004, was $3,301,000, as compared
to no
cost of revenues for the year ended December 31, 2003. Cost of revenues for
the
year ended December 31, 2004, was due to $3,269,000 in development expenses
for
HepeX-B that were incurred pursuant to our licensing agreement with Cubist,
as
well as due to $32,000 in licensing expense pursuant to our licensing agreement
with Yeda.
Research
and Development Costs.
Research and development costs decreased by $2,037,000 to $11,985,000 for the
year ended December 31, 2004, as compared to expenses of $14,022,000 for the
year ended December 31, 2003. The decrease in research and development costs
was
due primarily to the absence of approximately $1,919,000 in expenses related
to
early stage discovery research activities related to infectious diseases
(including an impairment charge of $354,000 in 2003), a $735,000 decrease in
expenses related to the development and clinical program of HepeX-B, due to
the
initiation of the collaboration agreement with Cubist and the subsequent
inclusion of development costs related to HepeX-B in Cost of Revenues above
and
a decrease of approximately $835,000 in expenses related to the XTL-6865
development and clinical program. This decrease was partially offset by an
approximate $1,452,000 increase in expenses associated with XTL-2125.
Participations.
There
were no participations from the Office of the Chief Scientist for the year
ended
December 31, 2004, as compared to participations of $3,229,000 in for the year
ended December 31, 2003. Participations received in 2003 were due to the Office
of the Chief Scientist’s decision to approve our grant applications that we had
submitted in 2003 and in 2002. We ceased requesting grants from the Office
of
the Chief Scientist in 2004 due to the potential contingent liability associated
with the transfer of manufacturing rights outside Israel.
General
and Administrative Expenses.
General
and administrative expenses increased by $1,029,000 to $4,134,000 for the year
ended December 31, 2004, as compared to expenses of $3,105,000 for the year
ended December 31, 2003. The increase in general and administrative expenses
was
due primarily to a $646,000 increase in payroll and related costs, which
included a $382,000 charge related to the termination of our former Chief
Executive Officer pursuant to his employment agreement as well to increased
expenses related to patent registration fees and professional fees.
Business
Development Costs.
Business development costs increased by $146,000 to $810,000 for the year ended
December 31, 2004, as compared to expenses of $664,000 for the year ended
December 31, 2003. The increase in business developments costs was due to a
$244,000 increase in professional fees primarily associated with our agreement
with Cubist that was signed in June 2004, offset by reduced travel-related
expenses.
Financial
Income.
Financial income for the year ended December 31, 2004, was $352,000, as compared
to financial income of $352,000 for the year ended December 31, 2003. Financial
income was flat due to reduced interest income earned on lower average cash
balances for the year ended December 31, 2004, as compared to the year ended
December 31, 2003, offset by an absence of foreign exchange losses which we
incurred in 2003.
Income
Taxes.
Income
tax expense decreased by $29,000 to $49,000 for the year ended December 31,
2004, as compared to expenses of $78,000 for year ended December 31, 2003.
Our
Income tax expense is attributable to taxable income from the continuing
operations of our subsidiary in the United States. This income is eliminated
upon consolidation of our financial statements.
Restructurings
2005
Restructuring
In
2005,
we implemented a restructuring plan designed to focus our resources on the
development of our lead programs, with the goal of moving these programs through
to clinical proof of concept. The 2005 restructuring included a 32 person
reduction in our workforce, 31 of whom were in research and development and
one
of whom was in general and administrative. As part of the 2005 restructuring,
we
took a charge in 2005 of $168,000, relating to employee dismissal costs,
$163,000 of which was included in research and development costs and $5,000
of
which was included in general and administrative expenses.
As
of
December 31, 2005, 28 employees have left under the 2005 restructuring plan
and
approximately $147,000 of dismissal costs have been paid. The other four
employees left in early 2006. As of December 31, 2005, approximately $21,000
in
employee dismissal obligations are included in accounts payable and accruals.
The balance of these obligations was paid in early 2006.
In
December 2005, as a result of our restructuring, and in accordance with the
provisions of FAS 144 “Accounting for the Impairment or Disposal of Long-Lived
Assets,” or FAS 144, we reviewed the carrying value of certain lab equipment
assets, and recorded an impairment charge in research and development costs
in
an amount of $26,000 in 2005.
2003
Restructuring
In
2003,
we implemented and completed a restructuring plan. As a result of this
restructuring, we ceased all early-stage discovery research activities related
to infectious diseases. The 2003 restructuring included a 20 person reduction
in
our workforce in Israel, 18 of whom were in research and development and two
of
whom were in general and administrative. As part of the 2003 restructuring,
we
took a charge in 2003 of $74,000, relating to employee dismissal costs, $58,000
of which was included in research and development costs and $16,000 of which
was
included in general and administrative expenses. We paid all of these amounts
in
2003. As part of the 2003 restructuring, we reevaluated our long-lived assets
in
accordance with FAS 144, and recorded a non-cash impairment charge of $354,000
in research and development costs for the year ended December 31,
2003.
Critical
Accounting Policies
The
discussion and analysis of our financial condition and results of operations
is
based upon our consolidated financial statements, which have been prepared
in
accordance with U.S. generally accepted accounting principles. The preparation
of these financial statements requires us to make estimates and judgments that
affect the reported amount of assets and liabilities and related disclosure
of
contingent assets and liabilities at the date of our financial statements and
the reported amounts of revenues and expenses during the applicable period.
Actual results may differ from these estimates under different assumptions
or
conditions.
We
define
critical accounting policies as those that are reflective of significant
judgments and uncertainties and which may potentially result in materially
different results under different assumptions and conditions. In applying these
critical accounting policies, our management uses its judgment to determine
the
appropriate assumptions to be used in making certain estimates. These estimates
are subject to an inherent degree of uncertainty. Our critical accounting
policies include the following:
Functional
Currency.
In
preparing our consolidated financial statements, we translate non-U.S. dollar
amounts in the financial statements into U.S. dollars. Under relevant accounting
guidance, the treatment of any gains or losses resulting from this translation
is dependent upon management’s determination of the functional currency. The
functional currency is determined based on management’s judgment and involves
consideration of all relevant economic facts and circumstances affecting our
business. Generally, the currency in which a company transacts a majority of
its
transactions would be considered the functional currency. The currency of the
primary economic environment in which our operations are conducted is the U.S.
dollar. We generate all of our revenues in U.S. dollars, and significant parts
of our operating expenses, capital expenditures, and external financings are
in
U.S. dollars. In addition, we hold most of our cash, cash equivalents, bank
deposits and marketable securities in U.S. dollars. Thus, our functional
currency is the U.S. dollar.
Since
the
U.S. dollar is the primary currency in the economic environment in which we
operate, monetary accounts maintained in currencies other than the U.S. dollar
(principally cash and liabilities) are re-measured using the representative
foreign exchange rate at the balance sheet date. Operational accounts and
non-monetary balance sheet accounts are measured and recorded at the rate in
effect at the date of the transaction.
Revenue
Recognition. We
recognize the revenue from our licensing agreement with Cubist under the
provisions of EITF 00-21 entitled “Revenue Arrangements with Multiple
Deliverables” and SAB 104 entitled “Revenue Recognition.” Under those
pronouncements, companies are required to allocate revenues from
multiple-element arrangements to the different elements based on sufficient
objective and reliable evidence of fair value. Since we have not been able
to
determine the fair value of each unit of accounting, the Cubist agreement was
accounted for as one unit of accounting, after failing the separation criteria.
We, therefore, recognize revenue on the Cubist agreement ratably over the life
of the arrangement. If actual future results vary, we may need to adjust our
estimates, which could have an impact on the timing and amount of revenue to
be
recognized.
In
addition, through 2005, Cubist has requested that we provide development
services that are reimbursed by them. As required by EITF 01-14 “Income
Statement Characterization of Reimbursements Received for “Out-of-Pocket”
Expenses Incurred,” amounts paid by us, as a principal, as “out-of-pocket” costs
are included in the cost of revenues as reimbursable out-of-pocket expenses,
and
the reimbursements we receive as a principal are reported as reimbursed
out-of-pocket revenues.
Stock
Compensation.
We have
granted options to employees, directors and consultants, as well as warrants
to
other third parties. Prior to January 1, 2005, we accounted for employee
stock-based compensation under the intrinsic value model in accordance with
Accounting Principles Board Opinion No. 25 - “Accounting for Stock Issued to
Employees,” or APB 25 and related interpretations. Under APB 25, compensation
expense is based on the difference, if any, on the date of the grant, between
the fair value of our ordinary shares and the exercise price. When the number
of
the underlying shares or the exercise price is not known at the grant date,
we
update, at each period, the compensation expenses until such data becomes known.
In addition, in accordance with Statement of Financial Accounting Standards
No.
123. “Accounting for Stock-Based Compensation,” or FAS 123, we disclosed pro
forma data assuming we had accounted for employee share option grants using
the
fair value-based method defined in FAS 123.
In
December 2004, the Financial Accounting Standards Board, or FASB, issued the
revised FAS No. 123 as Statements of Financial Accounting Standards No. 123R
“Share - Based Payment,” or FAS 123R, which addresses accounting for share-based
payment transactions in which a company obtains employee services in exchange
for (a) equity instruments of a company, or (b) liabilities that are based
on
the fair value of a company’s equity instruments or that may be settled by the
issuance of such equity instruments. In March 2005, the SEC issued Staff
Accounting Bulletin No. 107, or SAB 107, regarding the SEC's interpretation
of
FAS 123R.
FAS
123R
eliminates the ability to account for employee share-based payment transactions
using APB 25, and requires instead that such transactions be accounted for
using
the grant-date fair value based method. FAS 123R is effective as of the annual
reporting period that begins after June 15, 2005. Early adoption of FAS
123R is encouraged. FAS 123R applies to all awards granted or modified after
the
effective date of the standard. In addition, compensation cost for the unvested
portion of previously granted awards that remain outstanding on the effective
date shall be recognized on or after the effective date, as the related services
are rendered, based on the awards’ grant-date fair value as previously
calculated for the pro-forma disclosure under FAS 123.
We
implemented early adoption of FAS 123R, as of January 1, 2005, using the
modified prospective application transition method, as permitted by FAS 123R.
Under such transition method, our financial statements for periods prior to
the
effective date of FAS 123R (January 1, 2005) have not been restated. As a result
of the early adoption, we reduced the deferred share-based compensation against
the additional paid in capital.
The
fair
value of stock
options
granted
with service conditions was determined using the Black-Scholes valuation model,
which is consistent with our valuation techniques previously utilized for
options in footnote disclosures required under FAS 123, as amended by FAS
No. 148, “Accounting for Stock-Based Compensation - Transition and
Disclosure.” Such value is recognized as an expense over the service period, net
of estimated forfeitures, using the straight-line method under FAS 123R. The
fair value of stock options granted with market conditions, was determined
using
a lattice model that incorporated a Monte Carlo simulation method. Such value
is
recognized as an expense using the graded method under FAS123R.
The
estimation of stock awards that will ultimately vest requires significant
judgment, and to the extent actual results or updated estimates differ from
our
current estimates, such amounts will be recorded as a cumulative adjustment
in
the period those estimates are revised. We consider many factors when estimating
expected forfeitures, including types of awards, employee class, and historical
experience. Actual results, and future changes in estimates, may differ
substantially from our current estimates.
We
account for equity instruments issued to third party service providers (non
-
employees) in accordance with the fair value method prescribed by FAS123, and
as
of January 1, 2005, by FAS 123R, and the provisions of Emerging Issues Task
Force Issue No. 96-18, “Accounting for Equity Instruments That Are Issued to
Other Than Employees for Acquiring, or in Conjunction with Selling Goods or
Services,” or EITF 96-18.
Accounting
For Income Taxes.
In
preparing our consolidated financial statements, we are required to estimate
our
income taxes in each of the jurisdictions in which we operate. This process
requires management to estimate our actual current tax exposure and assess
temporary differences resulting from differing treatment of items for tax and
accounting purposes. These differences result in deferred tax assets and
liabilities. Deferred taxes are determined utilizing the asset and liability
method based on the estimated future tax effects of differences between the
financial accounting and tax bases of assets and liabilities under the
applicable tax laws. Deferred tax balances are computed using the tax rates
expected to be in effect when these differences reversed. Valuation allowances
are provided if, based upon the weight of available evidence, it is more likely
than not that some or all of the deferred tax assets will not be realized.
As a
result of our “approved enterprise” status, our current tax rate in Israel is
0%, and therefore no deferred tax assets have been included in these financial
statements in respect of carryforward losses. Our current income tax expense
results from taxes imposed on our U.S.-based subsidiary.
Paragraph
9(f) of Statement of Financial Accounting Standards No. 109, “Accounting for
Income Taxes,” or FAS 109, prohibits the recognition of deferred tax liabilities
or assets that arise from differences between the financial reporting and tax
bases of assets and liabilities that are measured from the local currency into
dollars using historical exchange rates and that result from changes in exchange
rates or indexing for tax purposes. Consequently, the above-mentioned
differences were not reflected in the computation of deferred tax assets and
liabilities.
Impairment.
Pursuant to FAS 144, long-lived assets, including certain intangible assets,
to
be held and used by an entity are reviewed for impairment whenever events or
changes in circumstances indicate that the carrying amount of the assets may
not
be recoverable. Under FAS 144, if the sum of the expected future cash flows
(undiscounted and without interest charges) of the long-lived assets held and
used is less than the carrying amount of such assets, an impairment loss would
be recognized, and the assets are written down to their estimated fair values.
Assets “held for sale” are reported at the lower of their carrying amount or
fair value less estimated costs to sell.
Accounting
Related to the Valuation of In-Process Research and Development.
In
accordance with FAS 142, we recorded a charge of $1,783,000 for the amount
allocated to in-process research and development in the VivoQuest transaction.
In-process research and development costs represent the relative fair value
of
purchased in-process research and development that, as of the transaction date,
have not reached technological feasibility and have no proven alternative future
use. As VivoQuest is a development stage enterprise that had not yet commenced
its planned principal operations, we accounted for the transaction as an
acquisition of assets pursuant to the provisions of FAS 142. Accordingly, the
purchase price was allocated to the individual assets acquired, based on their
relative fair values, and no goodwill was recorded.
The
fair
value of the in-process research and development acquired was estimated by
management with the assistance of an independent third-party appraiser, using
the “income approach.” In the income approach, fair value is dependent on the
present value of future economic benefits to be derived from ownership of an
asset. Central to this approach is an analysis of the earnings potential
represented by an asset and of the underlying risks associated with obtaining
those earnings. Fair value is calculated by discounting future net cash flows
available for distribution to their present value at a rate of return, which
reflects the time value of money and business risk. In order to apply this
approach, the expected cash flow approach was used. Expected cash flow is
measured as the sum of the average, or mean, probability-weighted amounts in
a
range of estimated cash flows. The expected cash flow approach focuses on the
amount and timing of estimated cash flows and their relative probability of
occurrence under different scenarios. The probability weighted expected cash
flow estimates are discounted to their present value using the risk free rate
of
return, since the business risk is incorporated in adjusting the projected
cash
flows to the probabilities for each scenario.
Recently
Issued Accounting Standards
FAS
No. 153, “Exchanges of Nonmonetary Assets - An Amendment of APB Opinion No. 29.”
In
December 2004, the FASB issued Statement of Financial Accounting Standards
No.
153, “Exchanges of Nonmonetary Assets - An Amendment of APB Opinion No. 29,” or
FAS 153. FAS 153 amends APB Opinion No. 29, “Accounting for Nonmonetary
Transactions,” or APB 29. The amendments made by FAS 153 are based on the
principle that exchanges of non-monetary assets should be measured based on
the
fair value of the assets exchanged. Further, the amendments eliminate the
exception for non-monetary exchanges of similar productive assets and replace
it
with a general exception for exchanges of non-monetary assets that do not have
commercial substance. The provisions in FAS 153 are effective for non-monetary
asset exchanges occurring in fiscal periods beginning after December 15, 2005
(January 1, 2006 for us). Early application of the FAS 153 is permitted. The
provisions of FAS 153 shall be applied prospectively. We do not expect the
adoption of FAS 153 to have a material effect on our financial statements or
our
results of operations.
FAS
No. 154, “Accounting Changes and Error Corrections.” In
May
2005, the FASB issued Statement of Financial Accounting Standards No. 154,
“Accounting Changes and Error Corrections,” or FAS 154. FAS 154 is a replacement
of APB Opinion No. 20, or APB 20, and FASB Statement No. 3. FAS 154 generally
requires retrospective application to prior periods' financial statements of
changes in accounting principle. Previously, APB 20 required that most voluntary
changes in accounting principle were recognized by including the cumulative
effect of changing to the new accounting principle in the net income of the
period of the change. FAS 154 applies to all voluntary changes in accounting
principle. It also applies to changes required by an accounting pronouncement
in
the unusual instance that the pronouncement does not include specific transition
provisions. When a pronouncement includes specific transition provisions, those
provisions should be followed. FAS 154 shall be effective for accounting changes
and corrections of errors made in fiscal years beginning after December15,
2005
(January 1, 2006 for us). We do not expect the adoption of FAS 154 to have
a
material effect on our financial statements or our results of
operations.
Impact
of Inflation and Currency Fluctuations
We
generate all of our revenues and hold most of our cash, cash equivalents, bank
deposits and marketable securities in U.S. dollars. While a substantial amount
of our operating expenses are in U.S. dollars, we incur a portion of our
expenses in New Israeli Shekels. In addition, we also pay for some of our
services and supplies in the local currencies of our suppliers. As a result,
we
are exposed to the risk that the U.S. dollar will be devalued against the New
Israeli Shekel or other currencies, and as result our financial results could
be
harmed if we are unable to guard against currency fluctuations in Israel or
other countries in which services and supplies are obtained in the future.
Accordingly, we may enter into currency hedging transactions to decrease the
risk of financial exposure from fluctuations in the exchange rates of
currencies. These measures, however, may not adequately protect us from the
adverse effects of inflation in Israel. In addition, we are exposed to the
risk
that the rate of inflation in Israel will exceed the rate of devaluation of
the
New Israeli Shekel in relation to the dollar or that the timing of any
devaluation may lag behind inflation in Israel. To date, our business has not
been materially adversely affected by changes in the U.S. dollar exchange rate
or by effects of inflation in Israel.
Governmental
Economic, Fiscal, Monetary or Political Policies that Materially Affected or
Could Materially Affect Our Operations
Israeli
companies are generally subject to income tax at the corporate tax rate of
31%
in 2006, which will be reduced as follows: 2007 - 29%, 2008 - 27%, 2009-26%,
2010 and after - 25%. However, we have been granted approved enterprise status,
and we are, therefore, eligible for a reduced corporate tax under the Law for
the Encouragement of Capital Investments, 1959. Subject to compliance with
applicable requirements, the portion of our undistributed profits derived from
the approved enterprise program will be tax-exempt for a period of two years
commencing in the first year in which we generate taxable income and will be
subject, for a period of five to eight years, to a reduced corporate tax of
between 10% and 25%, depending on the percentage of non-Israeli investors
holding our ordinary shares. The period of tax benefits with respect to our
approved enterprise program has not yet commenced because we have yet to realize
taxable income. However, this benefit period cannot extend beyond 12 years
from
the year of commencement of operations or 14 years from the year in which
approval was granted, whichever is earlier. If we subsequently pay a dividend
out of income derived from the “approved enterprise” during the tax exemption
period, it will be subject to tax on the amount distributed, including any
company tax on these amounts, at the rate which would have been applicable
had
such income not been exempt (25%). These benefits may not be applied to reduce
the U.S. federal tax rate for any income derived by our U.S. subsidiary. There
can be no assurance that such tax benefits will continue in the future at their
current levels or otherwise.
As
of
December 31, 2005, we did not have any taxable income. As of December 31, 2005,
our net operating loss carry-forwards for Israeli tax purposes amounted to
approximately $94 million. Under Israeli law, these net-operating losses may
be
carried forward indefinitely and offset against future taxable income, including
capital gains from the sale of assets used in the business, with no expiration
date.
For
a
description of Israeli government policies that affect our research and
development expenses, and the financing of our research and development, see
“Research and Development, Patents and Licenses - Israeli Government Research
and Development Programs” below.
Liquidity
and Capital Resources
We
have
financed our operations from inception primarily through our initial public
offering, various private placement transactions, our August 2004 placing and
open offer transaction and option and warrant exercises. As of December 31,
2005, we had received net proceeds of $45.7 million from our initial public
offering, net proceeds of $15.4 million from the 2004 placing and open offer
transaction, net proceeds of approximately $43.3 million from various private
placement transactions, and proceeds of $2.0 million from the exercise of
options and warrants.
As
of
December 31, 2005, we had $13.4 million in cash, cash equivalents, and
short-term bank deposits, a decrease of $9.5 million from December 31, 2004.
Cash used in operating activities for the year ended December 31, 2005, was
$10.5 million, as compared to $14.5 million for the year ended December 31,
2004. This decrease in cash used in operating activities was due primarily
to
reduced expenditures associated with the execution of our business plan,
pursuant to the 2005 restructuring. For the year ended December 31, 2005, net
cash used in investing activities of $9.5 million was primarily the result
of
liquidating short-term bank deposits. For the year ended December 31, 2005,
net
cash provided by financing activities of $1.5 million was the result of the
exercise of stock options in 2005.
Our
cash
and cash equivalents, as of December 31, 2005, were invested in highly
liquid investments such as cash and short-term bank deposits. As of December
31,
2005, we are unaware of any known trends or any known demands, commitments,
events, or uncertainties that will, or that are reasonably likely to, result
in
a material increase or decrease in our required liquidity. We expect that our
liquidity needs during 2006 will continue to be funded from existing cash,
cash
equivalents, short-term bank deposits and the proceeds from our recent private
placement.
Based
on
our current business plan, with the proceeds of our recent private placement
that closed in March 2006, we believe we have sufficient resources to fund
our
operations for approximately
the next 24 months. We
may
seek additional capital through a combination of public and private equity
offerings, debt financings and collaborative, strategic alliance and licensing
arrangements. We
have
made no determination at this time as to the amount, method or timing of any
such financing. Such
additional financing may not be available when we need it.
If we
are unable to obtain additional funds on terms favorable to us or at all, we
may
be required to cease
or
reduce our operating activities or sell or license to third parties some or
all
of our technology. If we raise additional funds by selling additional shares
of
our capital stock, the ownership interests of our shareholders will be diluted.
If we need to raise additional funds through the sale or license of our drug
candidates or technology, we may be unable to do so on terms favorable to us.
In
addition, see “Risk Factors - Risks Related to Our Financial
Condition.”
Our
forecast of the period of time through which our cash, cash equivalents and
short-term investments will be adequate to support our operations is a
forward-looking statement that involves risks and uncertainties. The actual
amount of funds we will need to operate is subject to many factors, some of
which are beyond our control. These factors include the following
|
·
|
the
timing of expenses associated with manufacturing and product development
of the proprietary drug candidates within our portfolio and those
that may
be in-licensed, partnered or acquired;
|
|
·
|
our
ability to achieve our milestones under licensing
arrangements;
|
|
·
|
the
timing of the in-licensing, partnering and acquisition of new product
opportunities; and
|
|
·
|
the
costs involved in prosecuting and enforcing patent claims and other
intellectual property rights.
|
We
have
based our estimate on assumptions that may prove to be inaccurate. We may need
to obtain additional funds sooner or in greater amounts than we currently
anticipate. Potential sources of financing may be obtained through strategic
relationships, public or private sales of our equity or debt securities, and
other sources. We may seek to access the public or private equity markets when
conditions are favorable due to our long-term capital requirements. We do not
have any committed sources of financing at this time, and it is uncertain
whether additional funding will be available when we need it on terms that
will
be acceptable to us, or at all. If we raise funds by selling additional shares
of our ordinary shares or other securities convertible into shares of our
ordinary shares, the ownership interest of our existing shareholders will be
diluted. If we are not able to obtain financing when needed, we may be unable
to
carry out our business plan. As a result, we may have to significantly limit
our
operations, and our business, financial condition and results of operations
would be materially harmed.
Off-Balance
Sheet Arrangements
We
have
not entered into any transactions with unconsolidated entities whereby we have
financial guarantees, subordinated retained interests, derivative instruments
or
other contingent arrangements that expose us to material continuing risks,
contingent liabilities, or any other obligations under a variable interest
in an
unconsolidated entity that provides us with financing, liquidity, market risk
or
credit risk support.
Quantitative
and Qualitative Disclosures about Market Risk
Interest
Rate Risk.
The
primary objective of our investment activities is to preserve principal while
maximizing our income from investments and minimizing our market risk. We invest
in government, investment-grade corporate debt securities, and bank deposits
in
accordance with our investment policy. Some of these instruments in which we
invest may have market risk. This means that a change in prevailing interest
rates may cause the principal amount of the investment to fluctuate. For
example, if we hold a security that was issued with a fixed interest rate at
the
then-prevailing rate and the prevailing interest rate later rises, the principal
amount of our investment will probably decline. As of December 31, 2005, our
portfolio of financial instruments consists of cash equivalents and short-term
bank deposits with multiple institutions. The average duration of all of our
investments held as of December 31, 2005, was less than one year. Due to the
short-term nature of these investments, we believe we have no material exposure
to interest rate risk arising from our investments.
Foreign
Currency and Inflation Risk.
We
generate all of our revenues and hold most of our cash, cash equivalents, bank
deposits and marketable securities in U.S. dollars. While a substantial amount
of our operating expenses are in U.S. dollars, we incur a portion of our
expenses in New Israeli Shekels. In addition, we also pay for some of our
services and supplies in the local currencies of our suppliers. As a result,
we
are exposed to the risk that the U.S. dollar will be devalued against the New
Israeli Shekel or other currencies, and as result our financial results could
be
harmed if we are unable to guard against currency fluctuations in Israel or
other countries in which services and supplies are obtained in the future.
Accordingly, we may enter into currency hedging transactions to decrease the
risk of financial exposure from fluctuations in the exchange rates of
currencies. These measures, however, may not adequately protect us from the
adverse effects of inflation in Israel. In addition, we are exposed to the
risk
that the rate of inflation in Israel will exceed the rate of devaluation of
the
New Israeli Shekel in relation to the dollar or that the timing of any
devaluation may lag behind inflation in Israel.
Obligations
and Commitments
As
of
December 31, 2005, we had known contractual obligations, commitments and
contingencies of $2,719,000. Of this amount, $652,000 relates to research and
development agreements, of which $585,000 is due within the next year, with
the
remaining balance due as per the schedule below. The additional $2,067,000
relates to our operating lease obligations, of which $720,000 is due within
the
next year, with the remaining balance due as per the schedule
below.
|
Payment
due by period
|
||||||||||||||||
|
Contractual
obligations
|
Total
|
Less
than
1
year
|
1-3
years
|
3-5
years
|
More
than
5
years
|
|||||||||||
|
Research
& development agreements
|
$
|
652,000
|
$
|
585,000
|
$
|
67,000
|
$
|
--
|
$
|
--
|
||||||
|
Operating
leases
|
2,067,000
|
720,000
|
921,000
|
426,000
|
--
|
|||||||||||
|
Total
|
$
|
2,719,000
|
$
|
1,305,000
|
$
|
988,000
|
$
|
426,000
|
$
|
--
|
||||||
Additionally,
we have undertaken to make contingent milestone payments to certain licensors
of
up to approximately $49.0 million over the life of the licenses, of which $34.0
million will be due upon or following regulatory approval of the drugs. In
some
cases, these contingent payments will only be triggered upon receipt of
royalties on sales of related products and in certain cases will partially
offset royalties we would otherwise owe those licensors. See “Business
-
Business Overview - License Agreements and Collaborations.”
We
also
have a commitment to make contingent payments to the Office of the Chief
Scientist of up to approximately $16.4 million, all of which is due from
royalties of approximately 3%-5% from proceeds from net sales of products in
the
research and development of which the Israeli government participated in by
way
of grants, as discussed in the immediately following section.
In
addition, in 2005, we received an assessment from the Israeli tax authorities
of
approximately $730,000 (including fines and interest expenses) related to
withholding taxes for taxable employee benefits and taxable income in Israel
paid to foreign companies during the periods of 2001-2004. We have recorded
an
accrual which we believe reflects the probable liability associated with this
assessment.
Research
and Development, Patents and Licenses
Research
and development costs consist primarily of salaries and related personnel costs,
fees paid to consultants and outside service providers for clinical and
laboratory development, facilities-related and other expenses relating to the
design, development, testing, and enhancement of our product candidates and
technologies.
The
following table sets forth the research and development costs for each of our
clinical-stage projects, our pre-clinical activities, and for all other research
and development programs for the periods presented.
|
Years
ended December 31,
|
|||||||||||||
|
2005
|
2004
|
2003
|
Cumulative,
as of December 31, 2005
|
||||||||||
|
XTL-2125
|
|||||||||||||
|
Research
and development costs
|
$
|
3,367,000
|
$
|
3,232,000
|
$
|
1,780,000
|
$
|
9,365,000
|
|||||
|
Less
participations
|
--
|
--
|
(168,000
|
)
|
(168,000
|
)
|
|||||||
|
3,367,000
|
3,232,000
|
1,612,000
|
9,197,000
|
||||||||||
|
XTL-6865
|
|||||||||||||
|
Research
and development costs
|
2,706,000
|
5,452,000
|
6,287,000
|
21,619,000
|
|||||||||
|
Less
participations
|
--
|
--
|
(1,459,000
|
)
|
(2,540,000
|
)
|
|||||||
|
2,706,000
|
5,452,000
|
4,828,000
|
19,079,000
|
||||||||||
|
HepeX-B1
|
|||||||||||||
|
Research
and development costs
|
2,743,000
|
6,570,000
|
4,036,000
|
26,985,000
|
|||||||||
|
Less
participations
|
(2,743,000
|
)
|
(3,269,000
|
)
|
(1,602,000
|
)
|
(10,173,000
|
)
|
|||||
|
|
--
|
3,301,000
|
2,434,000
|
16,812,000
|
|||||||||
|
Other
research and development programs2
|
|||||||||||||
|
Research
and development costs
|
1,240,000
|
--
|
1,919,000
|
30,933,000
|
|||||||||
|
Less
participations
|
--
|
--
|
--
|
(4,081,000
|
)
|
||||||||
|
1,240,000
|
--
|
1,919,000
|
26,852,000
|
||||||||||
|
Total
Research and development
|
|||||||||||||
|
Research
and development costs
|
10,056,000
|
15,254,000
|
14,022,000
|
88,902,000
|
|||||||||
|
Less
participations
|
(2,743,000)
|
(3,269,000)
|
(3,229,000
|
)
|
(16,962,000)
|
||||||||
|
7,313,000
|
11,985,000
|
10,793,000
|
71,940,000
|
||||||||||
____________________
1Includes
$6,012,000 in development costs for HepeX-B incurred from June 2004, the date
we
out-licensed HepeX-B to Cubist, for which we were subsequently reimbursed by
Cubist pursuant to our license agreement. The amount was classified in revenues
and cost of revenues in our statement of operations.
2Other
research and development programs includes DOS from September 2005 pursuant
to
the completion of the VivoQuest transaction and also includes early stage
discovery research activities that ceased in 2003.
Israeli
Government Research and Development Grants
In
the
past, we participated in programs offered by the Office of the Chief Scientist
under the Industry, Trade and Labor Ministry of Israel that support research
and
development activities. We received a grant from the Office of the Chief
Scientist for the year ended December 31, 2003 of $3,229,000. We did not apply
for, or receive, grants from the Office of the Chief Scientist for the years
2004 and 2005.
We
received grants from the Office of the Chief Scientist for several projects.
Under the terms of these grants, we will be required to pay a royalty ranging
between 3% to 5% of the net sales of products developed from an Office of the
Chief Scientist-funded project, beginning with the commencement of sales of
such
products and ending when 100% of the dollar value of the grant is repaid (100%
plus LIBOR interest applicable to grants received on or after January 1, 1999).
The royalty rate (between 3% and 5%) varies depending on the amount of years
that lapse between receipt of the grant and its repayment by us. At the time
grants were received, successful development of the related projects was not
assured. In the case of failure of a project that was partly financed, as above,
we are not obligated to pay any such royalties. At December 31, 2005, the
maximum amount of the contingent liability in respect of royalties related
to
ongoing projects including interest and LIBOR rate was equal to $3,778,000.
Israeli
law requires that the manufacture of products developed with government grants
be carried out in Israel, unless the Office of the Chief Scientist provides
a
special approval to the contrary. This approval, if provided, is generally
conditioned on an increase in the total amount to be repaid to the Office of
the
Chief Scientist to between 120% and 300% of the amount of funds granted. The
specific increase within this range would depend on the extent of the
manufacturing to be conducted outside of Israel. Alternatively, the restriction
on manufacturing outside of Israel shall not apply to the extent that plans
to
manufacture were disclosed when filing the application for funding (and provided
the application was approved based on the information disclosed in the
application). In such circumstances, the Office of the Chief Scientist will
take
into account the proposal that Office of the Chief Scientist-funded projects
will have an overseas manufacturing component. Under applicable Israeli law,
Israeli government consent is required to transfer to Israeli third parties
technologies developed under projects which the government funded. Transfer
of
Office of the Chief Scientist funded technologies outside of Israel is
prohibited. Israeli law further specifies that both the transfer of know-how
as
well as the transfer of intellectual property rights in such know-how are
subject to the same restrictions. These restrictions do not apply to exports
from Israel or the sale of products developed with these
technologies.
We
have
received the approval of the Office of the Chief Scientist for the transfer
of
manufacturing rights of our HepeX-B product under the terms of the agreement
with Cubist. As a consequence, we are obligated to repay the grants received
from the Office of the Chief Scientist for the financing of the HepeX-B product
from any amounts received by us from Cubist due to the sales of HepeX-B product,
at a percentage rate per annum calculated based on the aggregate amount of
grants received from the Office of the Chief Scientist divided by all amounts
invested by us in the research and development activities of HepeX-B, and up
to
an aggregate amount of 300% of the original amounts received for such project,
including interest at the LIBOR rate. As of December 31, 2005, the aggregate
amount received from the Office of the Chief Scientist for the financing of
the
HepeX-B project including interest and LIBOR rate was equal to $4,213,000.
At December 31, 2005, the maximum amount of the contingent liability in respect
of royalties related to HepeX-B product was $12,639,000.
Business
Overview
Introduction
We
are a
biopharmaceutical company engaged in the acquisition, development and
commercialization of pharmaceutical products for the treatment of infectious
diseases, particularly the treatment of hepatitis C.
We
currently have four products/programs under development:
|
·
|
XTL-2125
is
being developed for the treatment of hepatitis C. XTL-2125 is a novel
orally-available non-nucleoside HCV RNA polymerase inhibitor. XTL-2125
has
demonstrated potent activity against the hepatitis C virus in several
pre-clinical systems. IND-enabling GLP studies demonstrated that
XTL-2125
has favorable oral pharmacokinetics and a good safety profile in
multiple
animal species. We expect to commence a Phase I, placebo-controlled,
dose
escalation trial of XTL-2125 in chronic HCV patients in the first
half of
2006. The compound was in-licensed by us from B&C Biopharm Co., Ltd.,
a Korean drug development company.
|
|
·
|
XTL-6865
is
also being developed for the treatment of hepatitis C. XTL-6865 (formerly
known as the HepeX-C program) is a combination of two fully human
monoclonal antibodies (Ab68 and Ab65) against the hepatitis C virus
E2
envelope protein. The antibodies comprising XTL-6865 are expected
to
“trap” the virus in the patient’s serum and prevent the infection of
healthy liver cells. A single antibody version of this product was
tested
in a pilot clinical program that included both Phase I and Phase
II
clinical trials. In April 2005, we submitted an IND to the FDA in
order to
commence a Phase Ia/Ib clinical trial for XTL-6865, the dual-antibody
product. In September 2005, we announced the initiation of a Phase
Ia
clinical trial with XTL-6865 in patients with chronic hepatitis
C.
|
|
·
|
DOS
is
a pre-clinical program focused on the development of novel hepatitis
C
small molecule inhibitors. Compounds developed to date inhibit HCV
replication in a pre-clinical cell-based assay with potencies comparable
to clinical stage drugs. These compounds are presently being optimized.
We
expect to identify the first clinical candidate from the Diversity
Oriented Synthesis, or DOS, program and start IND-enabling GLP-safety
studies with this clinical candidate in the second half of 2006.
|
|
·
|
HepeX-B
is
being developed to prevent re-infection with hepatitis B, known as
HBV, in
liver transplant patients. HepeX-B is a mixture of two fully human
monoclonal antibodies, which bind to the HBV surface antigen, or
HBsAg. In
December 2005, data from the Phase IIb trial in liver transplant
patients
showed that patients treated with HepeX-B experienced no evidence
of viral
reinfection. Worldwide rights for HepeX-B were licensed to Cubist
in 2004,
in exchange for certain milestone payments and future royalties on
Cubist’s net sales. Cubist recently met with the FDA to discuss proposed
changes to the method of manufacture and formulation of HepeX-B.
Cubist is
expected to meet with the FDA again in the first half of 2006 to
discuss
the implications of these changes on the next stage of the clinical
program.
|
To
date,
we have not received approval for the sale of any of our drug candidates in
any
market and, therefore, have not generated any commercial revenues from the
sales
of our drug candidates. Moreover, preliminary results of our pre-clinical or
clinical tests do not necessarily predict the final results, and acceptable
results in early preclinical or clinical testing might not be obtained in later
clinical trials. Drug candidates in the later stages of clinical development
may
fail to show the desired safety and efficacy traits despite having progressed
through initial clinical testing. We have received license and reimbursed out
of
pocket expense revenue pursuant to our agreement with Cubist with respect to
HepeX-B, although HepeX-B has not yet been commercialized.
Our
Strategy
Under
our
current strategy, we plan to:
|
·
|
commence
the clinical development of XTL-2125;
|
|
·
|
continue
the clinical development of XTL-6865;
|
|
·
|
identify
clinical candidates from our DOS program and advance them into clinical
development; and
|
|
·
|
seek
to in-license or acquire additional
candidates.
|
Products
Under Development
We
are
developing several products for the treatment of hepatitis C. Chronic hepatitis
C is a serious life-threatening disease which affects around 170 to 200 million
people worldwide, according to a Datamonitor report from April 2005. We estimate
that between eight to 10 million of these people reside in the U.S., Europe
and
Japan. According to the BioSeeker Group, 20% to 30% of chronic hepatitis
patients will eventually develop progressive liver disease that may lead to
decomposition of the liver or hepatocellular carcinoma (liver cancer). According
to the National Digestive Diseases Information Clearing House (NDDIC), each
year
10,000 to 12,000 people die from HCV in the U.S. alone. The Centers for Disease
Control, or CDC, predicts, that by the end of this decade, the number of deaths
due to HCV in the U.S. will surpass the number of deaths due to
AIDS.
According
to the BioSeeker Group, the worldwide market for the treatment of chronic HCV
in
2003 was estimated at $3 billion and consists entirely of Interferon-based
treatments. Interferon alpha was first approved for use against chronic
hepatitis C in 1991. At present, the optimal regimen appears to be a 24 or
48
week course of the combination of Pegylated-Interferon and Ribavirin. In studies
done at the St. Louis University School of Medicine, a 24 week course of this
combination therapy yields a sustained response rate of approximately 40% to
45%
in patients with genotype 1 (the most prevalent genotype in the western world
according to the CDC) and a better sustained response with a 48 week course.
XTL-2125
XTL-2125
is a novel non-nucleoside HCV RNA polymerase inhibitor that is being developed
for the treatment of chronic hepatitis C. XTL-2125’s ability to inhibit HCV
replication was demonstrated in XTL's proprietary cell-based assay for HCV
infectivity. In addition, XTL-2125 was orally active in XTL’s proprietary
Trimera mouse model. IND-enabling GLP studies demonstrated that XTL-2125 has
a
favorable oral pharmacokinetics and a good safety profile in multiple animal
species.
In
the
third quarter of 2005, we filed an application with the Israel Ministry of
Health to conduct Phase I human trials of XTL-2125 in chronic HCV
patients. Patient dosing at several international sites is expected to
commence in the first half of 2006. This initial study will evaluate the safety,
pharmacokinetics and effects on viral load of single and multiple doses of
XTL-2125.
XTL-6865
XTL-6865
is being developed for the treatment of hepatitis C. XTL-6865 is a combination
of two fully human monoclonal antibodies (Ab68 and Ab65) against the hepatitis
C
virus E2 envelope protein. The antibodies comprising XTL-6865 are expected
to
“trap” the virus in the patient’s serum and prevent the infection of healthy
liver cells. A single antibody version of this product, then referred to as
HepeX-C, was tested in a pilot clinical program that included both Phase I
and
Phase II clinical trials. In April 2005, we submitted an IND to the FDA in
order
to commence a Phase Ia/Ib clinical trial for XTL-6865, the dual-antibodies
product. In September 2005, we announced the initiation of a Phase Ia clinical
trial with XTL-6865 in patients with chronic hepatitis C.
The
two
antibodies comprising XTL-6865 were selected by screening a large panel of
candidates based on their high level of activity against the virus in our
proprietary HCV models. We believe that a combination of two antibodies that
bind to different epitopes is essential to provide broad coverage of virus
quasispecies, and to minimize the probability for escape from therapy. We have
shown that the two antibodies chosen (Ab68 and Ab65) specifically bind and
immunoprecipitate viral particles from infected patients’ sera with different
HCV genotypes. In addition, both antibodies reduced mean viral load in
HCV-Trimera mice. We have also shown that incubation of an infectious human
serum with Ab68 or Ab65 prevented the serum’s ability to infect human liver
cells and human liver tissue.
The
current Phase Ia study is designed to evaluate the safety, tolerability, and
virologic activity of escalating single doses of XTL-6865 in patients with
chronic hepatitis C virus infection, and to assess the pharmacokinetics of
XTL-6865 in the presence of viral infection. The current study will be a
randomized, double blind, placebo-controlled, multi-center design. The following
XTL-6865 doses will be administered to groups of four patients each: 5 mg,
20
mg, 75 mg, 250 mg, 600 mg, 1200 mg, 2400 mg, and placebo. Within each group,
three subjects will receive XTL-6865 and one subject will receive placebo.
No
patient will be enrolled in more than one dose level. Up to two additional
groups of four patients may be enrolled at the current or intermediate doses
to
obtain additional safety or pharmacokinetic/pharmacodynamic data and to more
accurately define the Maximum Tolerated Dose (MTD). Concentrations of anti-E2
antibody and HCV RNA in the peripheral blood will be periodically
evaluated.
The
single antibody Hepex-C product candidate (Ab68) was tested in a pilot clinical
program, which included:
|
·
|
A
Phase Ia/Ib Clinical Program in Patients with Chronic
HCV,
which
demonstrated the safety and tolerability of using single and multi-doses
of Ab 68 up to 120mg for a 28 day dosing period. In terms of efficacy,
eight out of 25 patients had at least a 90% reduction in HCV-RNA
levels
from pre-treatment levels following administration of Ab68. These
trials
provided safety data, as well as a preliminary indication of anti-viral
activity in humans.
|
|
·
|
A
Phase IIa Clinical Trial with Ab68 Following Liver
Transplant,
which demonstrated the safety and tolerability of Ab68 up to 240mg
for a
12 week dosing period. The study was planned as a blinded,
placebo-controlled, dose-escalating study in a total of 24 liver
transplant patients receiving six different doses of Ab68 (20mg,
40mg,
80mg, 120mg, 240mg, and 480mg). Ab68 was administered once during
the
transplantation, then up to three times during the first 24 hours
following transplantation, then daily during the following six days,
and
then in decreasing frequency during the following eleven weeks. The
480mg
dose level was not tested due to a clinical hold as a result of an
intraoperative death of the first patient tested at the 480mg dose
level
(later determined by the medical examiner to be related to pulmonary
emboli (blood clots in the lung). The FDA later cleared the clinical
hold,
but we decided to discontinue the study and focus further development
efforts on the dual antibody product, XTL-6865. No other drug-related
serious adverse events were reported during this study.
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During
the period of daily dosing (the first seven days following the
transplant), reduction in viral load from baseline were greater in
the two
highest dose groups (120 mg and 240 mg) compared to the placebo group.
On
day one following the transplant (when Ab68 was administered three
times)
the median reduction in viral load from baseline of the highest dose
group
(240mg) was 1-log (90%) greater than the placebo group. The 120mg
and
240mg dose groups had a greater reduction in viral load than the
placebo
group during the first week when dosed daily. This effect was less
evident
when dosed less frequently than daily. This data provided additional
evidence of anti-viral activity in immunosuppressed patients. It
should be
noted that the small number of patients in this pilot study did not
allow
us to draw statistical analysis.
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DOS
DOS
is a
pre-clinical program focused on the development of three families of novel
hepatitis C small molecule inhibitors. Compounds in each family inhibit
HCV replication in a pre-clinical cell-based assay with potencies comparable
to
clinical stage drugs. These compounds are presently being optimized. We
expect to identify the first clinical candidate from the DOS program and start
IND-enabling GLP-safety studies with this clinical candidate in the second
half
of 2006.
We
gained
access to the DOS program through a license and asset purchase agreement with
VivoQuest Inc. that was completed in September 2005. Under this agreement,
we
licensed lead HCV molecules, a proprietary compound library and medicinal
chemistry technologies. The DOS small molecule chemistry
technology developed at VivoQuest was used to create these molecules and is
currently being used to produce optimized compounds for advanced pre-clinical
and IND-enabling GLP safety studies. See “Business-Material
Contracts.”
HepeX-B
HepeX-B
is being developed to prevent re-infection with HBV in liver transplant
patients. Protection of the transplanted liver from recurrent HBV infection
is
critical to preserving graft function. Life-long HBV prophylactic treatment
is
typically necessary, since the virus remains in several other body compartments
following removal of the infected liver. Without treatment, Hepatitis B
infection of the transplanted liver reoccurs rapidly resulting in progressive
disease, graft failure, and death.
HepeX-B
is a mixture of two fully human monoclonal antibodies which bind to the HBV
surface antigen, or HBsAg. HepeX-B is being developed as an alternative to
the
present standard-of-care, hepatitis B Immunoglobulin, or HBIg, which has several
disadvantages, among them complicated and uncomfortable patient administration
(intravenous or painful intra-muscular injection). In addition, as HepeX-B
is
not isolated from human blood, risk of infection from blood-borne organisms
is
minimal. The present market size of HBIg is estimated to be about $100 million
per year worldwide.
HepeX-B
was recently studied in a Phase IIb clinical trial in liver transplant patients.
In the Phase IIb study, HepeX-B was studied as maintenance therapy to prevent
reinfection with hepatitis B in liver transplant patients. The data from the
Phase IIb study was derived from patients who had completed at least six months
of therapy, which was the treatment duration at which the primary endpoint
was
measured. Eleven patients received monthly 20 mg infusions of HepeX-B; ten
received monthly infusions of 40 mg HepeX-B; and nine received monthly infusions
of 5000 IU HBIg (current standard of care). Data from liver transplant patients
who were treated with monthly infusions of 20 or 40 mg HepeX-B versus 5000
IU of
HBIg showed that patients with either dose of HepeX-B experienced no evidence
of
viral reinfection. The data also showed fewer and less serious adverse
experiences reported in both HepeX-B groups as compared to the HBIg group,
although the differences were not statistically significant given the number
of
patients in the trial. Patients who were treated with HepeX-B as well as HBIg
also received concurrent HBV polymerase inhibitor.
Prior
to
the initiation of the Phase IIb study in liver transplant patients, we conducted
a Phase I clinical study in twelve healthy volunteers to determine the
pharmacokinetic properties of HepeX-B. The study evaluated a single intravenous
infusion of 10mg or 40mg of HepeX-B with subsequent follow-up over a 12-week
period. HepeX-B was well tolerated by all subjects. Although our study did
not
directly compare HepeX-B to HBIg, the trough antibody concentrations achieved
with 10mg and 40mg doses of HepeX-B were similar to or higher than
concentrations achieved with standard doses of HBIg used in current treatment
protocols (10,000mg), thus potentially enabling the development of a low volume,
“patient friendly” formulation.
Orphan
drug status, a regulatory designation that provides exclusive marketing rights
to drug candidates that would not otherwise be commercially viable, has been
granted for HepeX-B in the U.S. and Europe.
In
June
2004, we announced the completion of a license agreement with Cubist for the
worldwide development and commercialization of HepeX-B. Under this agreement,
as
amended, we were responsible for certain clinical and product development
activities of HepeX-B through August 2005, at the expense of Cubist. We have
transferred full responsibility for completing the development of HepeX-B to
Cubist. Cubist will be responsible for completing the development and for
registration and commercialization of the product worldwide. Under the terms
of
the agreement, as amended, Cubist paid us an initial up-front payment of $1
million upon the signing of the agreement, a further aggregate amount of $1
million as collaboration support was paid in 2004, and an additional amount
of
up to $3 million will be paid upon achievement of certain regulatory milestones.
Under the agreement, we are entitled to receive royalties from net sales by
Cubist, generally ranging from 10% to 17%. In the event that the actual costs
incurred in conducting activities that Cubist determines are necessary or
advisable to obtain regulatory approval for HepeX-B for the prevention of
recurrent hepatitis B infections in liver transplant patients exceed $33.9
million, any costs in excess shall be borne in equal share by us and
Cubist.
Cubist
recently met with the FDA to discuss proposed changes to the method of
manufacture and formulation of HepeX-B. Specifically, Cubist plans to shift
from
the use of hybridoma cells to Chinese Hamster Ovary (CHO) cells and to switch
to
subcutaneous delivery prior to Phase III. The objective of the manufacturing
change is to provide a stable platform for commercialization. The switch to
subcutaneous administration is meant to increase patient convenience and
compliance with chronic therapy. Cubist will meet again with the FDA in the
first-half of 2006 to discuss the implications of these changes on the next
stage of the clinical program.
Proprietary
Technology
Our
proprietary Trimera technology is a method for introducing functional human
cells or tissue into a mouse. The Trimera technology is a patented tool whereby
murine immune systems are ablated by radiation, and bone marrow is transplanted
from genetically immuno-deficient mice to re-enable red blood cell production.
The result is the production of “radiation chimeras.” As these chimeras have no
immune system, they are able to accept implanted human cells, without rejection,
thereby creating a “Trimera.” The resulting mouse can be used:
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·
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to
generate humanized monoclonal antibodies, or hMAbs (the “Trimera hMAb
Technology”); and/or
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|
·
|
as
an animal model of human disease (the “Trimera Model Technology”).
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These
models can be used for testing various approaches to treat human disease,
including the development of new prophylactic and therapeutic products and
have
been used to discover the HepeX-B product and to screen the activity of XTL-6865
and XTL-2125.
Intellectual
Property and Patents
General
Patents
and other proprietary rights are very important to the development of our
business. We will be able to protect our proprietary technologies from
unauthorized use by third parties only to the extent that our proprietary rights
are covered by valid and enforceable patents or are effectively maintained
as
trade secrets. It is our intention to seek and maintain patent and trade secret
protection for our drug candidates and our proprietary technologies. As part
of
our business strategy, our policy is to actively file patent applications in
the
U.S. and internationally to cover methods of use, new chemical compounds,
pharmaceutical compositions and dosing of the compounds and compositions and
improvements in each of these. We also rely on trade secret information,
technical know-how, innovation and agreements with third parties to continuously
expand and protect our competitive position.
Generally,
patent applications in the U.S. are maintained in secrecy for a period of
18 months or more. Since publication of discoveries in the scientific or
patent literature often lag behind actual discoveries, we are not certain that
we were the first to make the inventions covered by each of our pending patent
applications or that we were the first to file those patent applications. The
patent positions of biotechnology and pharmaceutical companies are highly
uncertain and involve complex legal and factual questions. Therefore, we cannot
predict the breadth of claims allowed in biotechnology and pharmaceutical
patents, or their enforceability. To date, there has been no consistent policy
regarding the breadth of claims allowed in biotechnology patents. Third parties
or competitors may challenge or circumvent our patents or patent applications,
if issued. Granted patents can be challenged and ruled invalid at any time,
therefore the grant of a patent is not of itself sufficient to demonstrate
our
entitlement to a proprietary right. The disallowance of a claim or invalidation
of a patent in any one territory can have adverse commercial consequences in
other territories.
If
our
competitors prepare and file patent applications in the United States that
claim
technology also claimed by us, we may choose to participate in interference
proceedings declared by the United States Patent and Trademark Office to
determine priority of invention, which could result in substantial cost, even
if
the eventual outcome is favorable to us. While we have the right to defend
patent rights related to our licensed drug candidates and technologies, we
are
not obligated to do so. In the event that we decide to defend our licensed
patent rights, we will be obligated to cover all of the expenses associated
with that effort. Because of the extensive time required for development,
testing and regulatory review of a potential product, it is possible that before
we commercialize any of our products, any related patent may expire or remain
in
existence for only a short period following commercialization, thus reducing
any
commercial advantage or financial value attributable to the patent.
If
patents are issued to others containing preclusive or conflicting claims and
these claims are ultimately determined to be valid, we may be required to obtain
licenses to these patents or to develop or obtain alternative technology. Our
breach of an existing license or failure to obtain a license to technology
required to commercialize our products may seriously harm our business. We
also
may need to commence litigation to enforce any patents issued to us or to
determine the scope and validity of third-party proprietary rights. Litigation
would create substantial costs. An adverse outcome in litigation could subject
us to significant liabilities to third parties and require us to seek licenses
of the disputed rights from third parties or to cease using the technology
if
such licenses are unavailable.
XTL-2125
One
patent family presently covers XTL-2125. It covers the structure of the
compound, and its use for the treatment of chronic HCV patients. The patent
application covers the unique structure of the molecules and their use as a
pharmaceutical composition for the treatment of HCV. This patent family, if
issued, will expire in 2023. Based on the provisions of the Patent Term
Extension Act, we currently believe that we would qualify for certain patent
term extensions. The patent application covering XTL-2125 is exclusively
licensed to us by B&C Biopharm Co., Ltd.
XTL-6865
XTL-6865
is a combination of two human monoclonal antibodies against HCV, Ab68 and Ab65.
Three patent families presently cover XTL-6865, including the two human
monoclonal antibodies comprising XTL-6865 and its use to treat HCV infection.
The patents cover both the treatment of chronic HCV patients with the antibodies
and the prevention of liver re-infection in liver transplant recipients. One
family concerns one antibody comprising XTL-6865, Ab68. Two families concern
the
second antibody comprising XTL-6865, Ab65.
The
patent and patent applications covering Ab68 are exclusively licensed to us
from
the DRK-Blutspendedienst Baden-Wurttemberg (Ulm University, Ulm, Germany).
The
patent and patent applications covering Ab65 are exclusively licensed to us
from
Stanford University, California in all territories outside China, and in China,
it is co-exclusively licensed to us and Applied Immunogenetics.
Currently,
XTL-6865 and its use to treat hepatitis C infection is covered by one issued
U.S. patent that will expire in 2019. Additional patent applications, if issued,
will expire between 2019 and 2021. Based on the provisions of the Patent Term
Extension Act, we currently believe that we would qualify for certain patent
term extensions. We believe that we will have sufficient time to commercially
utilize the inventions directed to the treatment and prevention of hepatitis
C
infection.
HepeX-B
Three
patent families presently cover HepeX-B, including the two human monoclonal
antibodies comprising HepeX-B and its use to treat HBV infection. The patents
and patent applications cover both the treatment of chronic HBV patients with
the antibodies and the prevention of liver re-infection in liver transplant
recipients. Two of the families correspond each to a separate antibody
comprising HepeX-B, with one family owned by us, and the second family jointly
owned by Yeda and us. A third family of patent applications concerns treatment
of HBV patients with the combination of the antibodies and is owned by us.
Currently,
HepeX-B and its use to treat hepatitis B infection is covered by several issued
patents that will expire in 2017. The patents applications covering the
combination of antibodies, if issued, will expire in 2021. Based on the
provisions of the Patent Term Extension Act, we currently believe that we would
qualify for certain patent term extensions. We believe that we will have
sufficient time to commercially utilize the inventions directed to the treatment
and prevention of hepatitis B infection in liver transplant
patients.
DOS
The
lead
molecules that are included in the VivoQuest license are covered by two issued
patents and four patent applications. The patent applications describe both
the
structure of the compounds and their use for treating HCV infection. The two
issued VivoQuest patents will expire in 2023. Additional patent applications,
if
issued, will expire in 2023, 2024 and 2025. Based on the provisions of the
Patent Term Extension Act, we currently believe that we would qualify for
certain patent term extensions.
We
believe that we will have sufficient time to commercially utilize the inventions
from our small molecule development program directed to the treatment and
prevention of hepatitis C infection.
Trimera
Technology
Three
patent families presently cover the Trimera technology, each covering a
different use of the basic technology. The patents cover the Trimera mouse,
a
method for its production, and its various applications. The patents are
exclusively licensed to us by Yeda.
Currently,
the Trimera mouse and its various applications are covered by several issued
patents that will expire between 2010 and 2015. The patents covering the
hepatitis animal model will expire between 2012 and 2016. We believe that we
will have sufficient time to commercially utilize the inventions resulting
from
the Trimera technology.
Other
Intellectual Property Rights
We
depend
upon trademarks, trade secrets, know-how and continuing technological advances
to develop and maintain our competitive position. To maintain the
confidentiality of trade secrets and proprietary information, we require our
employees, scientific advisors, consultants and collaborators, upon commencement
of a relationship with us, to execute confidentiality agreements and, in the
case of parties other than our research and development collaborators, to agree
to assign their inventions to us. These agreements are designed to protect
our
proprietary information and to grant us ownership of technologies that are
developed in connection with their relationship with us. These agreements may
not, however, provide protection for our trade secrets in the event of
unauthorized disclosure of such information.
In
addition to patent protection, we may utilize orphan drug regulations to provide
market exclusivity for certain of our drug candidates. The orphan drug
regulations of the FDA provide incentives to pharmaceutical and biotechnology
companies to develop and manufacture drugs for the treatment of rare diseases,
currently defined as diseases that exist in fewer than 200,000 individuals
in
the United States, or, diseases that affect more than 200,000 individuals in
the
United States but that the sponsor does not realistically anticipate will
generate a net profit. Under these provisions, a manufacturer of a designated
orphan drug can seek tax benefits, and the holder of the first FDA approval
of a
designated orphan product will be granted a seven-year period of marketing
exclusivity for such FDA-approved orphan product. We believe that certain of
the
indications for our drug candidates will be eligible for orphan drug
designation.
Licensing
Agreements and Collaborations
We
have
formed strategic alliances with a number of companies for the manufacture and
commercialization of our products. Our current key strategic alliances are
discussed below.
XTL-2125
License
XTL-2125
has been licensed from B&C Biopharm Co., Ltd., or B&C, since February
2003. Under the terms of the agreement, we have exclusive rights to XTL-2125
worldwide, with the exception of Asia, which is shared between the two
companies, and Korea, for which B&C retains exclusive rights. Under the
terms of the agreement, we are obligated to make certain milestone payments
in
addition to royalties on product sales. To date we have made $1.1 million in
license and milestone payments to B&C, and we have agreed to make contingent
milestone payments of up to approximately $13.4 million over the life of the
license, of which $8.0 million will be due upon or following regulatory approval
of the drug. The license terminates upon the expiration of the last of the
licensed patents. Notwithstanding the above, we may terminate this agreement
upon specified notice to B&C.
XTL-6865
License
XTL-6865
is a combination of two human monoclonal antibodies against HCV, Ab68 and
Ab65.
In
April
2000, we licensed Ab68 under an exclusive worldwide license from the
DRK-Blutspendedienst Baden-Wurttemberg (Ulm University, Germany, or Ulm). Under
the terms of this agreement, we are obligated to pay Ulm a specified royalty
rate on sales of product incorporating Ab68. We can deduct certain payments
that
are made to third parties from these royalties, subject to a minimum royalty
rate. We are also obligated to pay Ulm a specified percentage of any milestone
payments we may receive from any sublicensee to whom we may grant a license
or
sublicense of Ab68 or technology related to the production of Ab68. We can
deduct certain of these payments that are made to third parties from the
percentage of milestone payments owed to Ulm, subject to a minimum milestone
payment amount. Either party may terminate the agreement, by written notice,
upon or after the winding up or insolvency of the other party, or upon or after
commitment of a material breach by the other party that cannot be cured, or
if
curable, has not been cured, within 60 days after receipt of notice. In the
absence of such termination, the agreement shall expire upon the expiration
of
the license granted under the agreement. To date we have made $150,000 in
license and milestone payments to Ulm.
In
September 2003, we licensed Ab65 from Stanford University under an exclusive
license agreement. Under the terms of this agreement, we have exclusive rights
to Ab65 worldwide, excluding China. In China, we have co-exclusive rights with
Applied Immunogenetics LLC. Under the terms of this agreement, we must use
commercially reasonable efforts to commercialize and market Ab65. We are
obligated to make royalty payments to Stanford University on sales of product
incorporating Ab65, and we are also obligated to make milestone payments upon
the occurrence of certain specified events. To date we have made $182,000 in
license and milestone payments to Stanford University, and we have undertaken
to
make contingent milestone payments of up to approximately $200,000 over the
life
of the license, all of which will be due upon or following regulatory approval
of the drug. The license terminates upon the later of the expiration of last
of
the licensed patents or at the time of our last royalty payment. Notwithstanding
the above, we may terminate this agreement upon specified notice to Stanford
University. In addition, should we fail to meet certain developmental milestones
for Ab65, our rights to the use of Ab65 become non-exclusive upon notice to
that
effect to us by Stanford University.
In
addition, under an agreement entered into in September 2003, we are obligated
to
make royalty payments on sales of product incorporating Ab65 to Applied
Immunogenetics LLC, a company that previously held non-exclusive rights to
Ab65
and returned them to Stanford University, enabling us to gain exclusive rights
to Ab65 from Stanford University. Our agreement with Applied Immunogenetics
LLC
expires on the expiration or termination of our exclusive agreement with
Stanford University, as described above. To date we have made $183,000 in
license and milestone payments to Applied Immunogenetics LLC. There are no
additional contingent milestone payments.
Cubist
License
We
have
entered into a licensing agreement with Cubist dated June 2, 2004, as amended,
under which we granted to Cubist an exclusive, worldwide license (with the
right
to sub-license) to commercialize HepeX-B and any other product containing a
hMAb
or humanized monoclonal antibody or fragment directed at the hepatitis B virus
owned or controlled by us. Under this agreement, we were responsible for certain
clinical and product development activities of HepeX-B through August 2005,
at
the expense of Cubist. We have transferred full responsibility for completing
the development of HepeX-B to Cubist. Cubist will be responsible for completing
the development and for registration and commercialization of the product
worldwide. Nevertheless, during the term of this agreement, we have an ongoing
obligation to transfer to Cubist all information Cubist may reasonably require
and to provide Cubist with reasonable access to pertinent employees of ours
that
have experience with or information related to HepeX-B. We are also required
to
file, prosecute and maintain the relevant patents at our sole
expense.
In
the
event that the actual costs incurred in conducting activities that Cubist
determines are necessary or advisable to obtain regulatory approval for HepeX-B
for the prevention of recurrent hepatitis B infections in liver transplant
patients exceed $33.9 million, any costs in excess shall be borne in equal
share
by us and Cubist. Under the terms of the agreement, Cubist paid us an initial
up-front payment of $1 million upon the signing of the agreement, a further
aggregate amount of $1 million as collaboration support was paid in 2004, and
an
additional amount of up to $3 million will be paid upon achievement of certain
regulatory milestones. We are entitled to receive royalties from net sales
by
Cubist, generally ranging from 10% to 17%, depending on levels of net sales
achieved by Cubist, subject to certain deductions based on patent protection
of
HepeX-B in that territory, total costs of HepeX-B development, third party
license payments and indemnification obligations.
Cubist
has the right to sub-license HepeX-B. The sub-licensee fees we will receive
in
such cases will vary according to the territory, the subject of the sub-license,
the patent protection of HepeX-B in that territory, total costs of HepeX-B
development, third party license payments, indemnification obligations and
local
competition. For example, where HepeX-B is not patent protected and a competing
product obtains more than an agreed percentage of the local market, we would
receive no royalties on sales of HepeX-B.
Cubist
has granted us the non-exclusive right of negotiation during the term of the
agreement to obtain all or any portion of the rights to manufacture and supply
HepeX-B or any other product containing an hMAb or humanized monoclonal antibody
or fragment directed at the hepatitis B virus owned or controlled by us.
Furthermore, in certain circumstances, we have the exclusive right to negotiate
with Cubist to obtain from Cubist a sub-license to market and sell the HepeX-B
or such other product in certain territories.
We
agreed
that during the term of the agreement and for one year thereafter, we will
not
research, develop or commercialize any competitive product containing a human
or
humanized monoclonal antibody or fragment that is directed to and binds with
the
hepatitis B virus.
The
agreement expires on the later of the last valid patent claim covering HepeX-B
to expire or 10 years after the first commercial sale of HepeX-B on a
country-by-country basis.
VivoQuest
License
In
August
2005, we entered into a license agreement with VivoQuest covering a proprietary
compound library, including certain HCV compounds. Under the terms of the
license agreement, we have exclusive worldwide rights to VivoQuest’s
intellectual property and technology in all fields of use. To date we have
made
approximately $0.9 million in license payments to VivoQuest under the license
agreement The license agreement also provides for additional milestone payments
triggered by certain regulatory and sales targets. These additional milestone
payments total $34.6 million, $25.0 million of which will be due upon or
following regulatory approval or actual product sales, and are payable in cash
or ordinary shares at our election. In addition, the license agreement requires
that we make royalty payments to VivoQuest on product sales.
Yeda
License
In
April
of 1993, we entered into a research and license agreement with Yeda, which
we
refer to as the Yeda Agreement, under which Yeda granted us an exclusive
worldwide license to use the Trimera patent portfolio and to exclusively use
the
information derived from the performance of certain research for the purposes
specified in the agreement in any country where a licensed patent covers a
product sold under the license or other licensed activity until the date on
which the last licensed patent expires or until 12 years from the later of
the
first commercial sale of a product (or first receipts to us from other licensed
activity) in such country, and in any other country until 12 years from the
first commercial sale of a product (or first receipts to us from other licensed
activity) in that country. Under the agreement, any assignment of the license
granted by Yeda requires Yeda's prior written consent.
The
Yeda
Agreement has undergone a number of amendments, one of the end results of which
is that we shall pay to Yeda the following fees: a royalty of 3% of all net
sales received by us; 25% of amounts received by us on net sales of third
parties (less certain royalties payable by us to third parties), but no more
than 3% and no less than 1.5% of such net sales; and a royalty ranging between
20% to 40% on any receipts to us other than our net sales or receipts on net
sales made by third parties. Furthermore, such amendments have also changed
the
termination provisions relating to Yeda’s entitlement to terminate the agreement
if we do not pay Yeda a certain minimum amount of annual royalties of $100,000
or $200,000, depending on the year. We may terminate the agreement with Yeda
with six months advance notice in which event our rights in any technology
licensed by Yeda to us shall terminate and any technology derived from research
and development activities performed by us in connection with the technology
licensed by Yeda to us shall vest in Yeda.
In
the
most recent amendment of the Yeda Agreement, in order to facilitate the grant
of
the license by us to Cubist under the terms of the HepeX-B collaboration, Yeda
received the right to receive at least 1.5% of net sales of HepeX-B by Cubist
sub-licensees, regardless of the amount received by us from Cubist in respect
of
such sales.
Competition
Competition
in the pharmaceutical and biotechnology industries is intense. Our competitors
include pharmaceutical companies and biotechnology companies, as well as
universities and public and private research institutions. In addition,
companies that are active in different but related fields represent substantial
competition for us. Many of our competitors have significantly greater capital
resources, larger research and development staffs and facilities and greater
experience in drug development, regulation, manufacturing and marketing than
we
do. These organizations also compete with us to recruit qualified personnel,
attract partners for joint ventures or other collaborations, and license
technologies that are competitive with ours. To compete successfully in this
industry we must identify novel and unique drugs or methods of treatment and
then complete the development of those drugs as treatments in advance of our
competitors.
The
drugs
that we are attempting to develop will have to compete with existing therapies.
In addition, a large number of companies are pursuing the development of
pharmaceuticals that target the same diseases and conditions that we are
targeting. Other
companies have products or
drug
candidates in various stages of pre-clinical or clinical development to treat
diseases for which we are also seeking to discover and develop drug candidates.
Some of these potential competing drugs are further advanced in development
than
our drug candidates and may be commercialized earlier.
Competing
Products for Treatment of Chronic Hepatitis C
We
believe that a significant number of drugs are currently under development
that
will become available in the future for the treatment of
hepatitis C.
At
present, the only approved therapies for treatment of chronic HCV are
Interferon-based. There are multiple drugs presently under development for
the
treatment of HCV, most of which are in the pre-clinical or early stage of
clinical development. These compounds are developed by both established
pharmaceutical companies, as well as by biotech companies. Examples of such
companies are: Anadys Pharmaceuticals, Inc., F. Hoffman-LaRoche & Co.,
Intercell AG, Schering-Plough Corporation, Gilead Sciences, Inc., Idenix
Pharmaceuticals, Inc., InterMune, Inc. and Vertex Pharmaceuticals Incorporated.
Many of these companies and organizations, either alone or with their
collaborative partners, have substantially greater financial, technical and
human resources than we do. In addition, our competitors also include smaller
private companies such as Pharmasset, Ltd.
Competing
Products for Preventing Re-Infection with Hepatitis B in Liver Transplant
Patients
The
present standard-of-care for preventing hepatitis B in liver transplant patients
is Hepatitis B Immune Globulin, or HBIg. Our strategy is to replace the existing
standard of care with HepeX-B.
Key
producers of HBIg in the U.S. are NABI Biopharmaceuticals Inc., Bayer Biological
Products, a division of Bayer Healthcare, and Cangene Corporation. Key HBIg
producers in the European Union, or E.U., are Biotest AG, ZLB Behring, a
subsidiary of CSL Ltd., and Berna Biotech AG. We are not aware of any competing
monoclonal antibody against HBV currently in clinical development.
Several
small molecules against HBV are presently being used in liver transplant
patients. They presently include Lamivudine, a product of GlaxoSmithKline PLC,
and Hepsera, a product of Gilead Sciences Inc., and may include additional
small
molecule drugs presently in Phase III clinical trials. These drugs are commonly
prescribed in combination with HBIg, and not as a replacement. However, several
centers have terminated HBIg use and maintain patients on small molecule therapy
alone. To our knowledge, the impact of this approach on efficacy has not been
established.
Supply
and Manufacturing
We
currently have no manufacturing capabilities and do not intend to establish
any
such capabilities.
XTL-2125
In
2003,
we entered into a contract manufacturing agreement with an Israeli-based
manufacturer for the supply of XTL-2125. We believe that this contract
manufacturer will be adequate to satisfy our current pre-clinical and planned
clinical supply needs.
XTL-6865
In
2000,
we entered into a contract manufacturing agreement with a U.S.-based
manufacturer for the supply of the HepeX-C drug product, the single antibody
version of XTL-6865, and subsequently under a master agreement for the supply
of
XTL-6865, the dual-MAb product. We believe that this contract manufacturer
will
be adequate to satisfy our current clinical supply needs. For commercial supply
of XTL-6865, we intend to contract with a manufacturer to develop a robust
validated production process for large scale drug supply.
HepeX-B
Future
supply of the HepeX-B clinical material will be manufactured by a contract
manufacturer to be selected by our partner Cubist. Cubist recently met with
the
FDA to discuss proposed changes to the method of manufacture and formulation
of
HepeX-B. Cubist will meet again with the FDA in the first-half of 2006 to
discuss the implications of these changes on the next stage of the clinical
program.
DOS
For
planned pre-clinical and clinical supply of the HCV compounds licensed from
VivoQuest, we intend to enter into a contract with a manufacturer to produce
our
pre-clinical and clinical supply needs.
General
At
the
time of commercial sale, to the extent possible and commercially practicable,
we
plan to engage a back-up supplier for each of our product candidates. Until
such
time, we expect that we will rely on a single contract manufacturer to produce
each of our product candidates under cGMP regulations. Our third-party
manufacturers have a limited numbers of facilities in which our product
candidates can be produced and will have limited experience in manufacturing
our
product candidates in quantities sufficient for conducting clinical trials
or
for commercialization. Our third-party manufacturers will have other clients
and
may have other priorities that could affect our contractor’s ability to perform
the work satisfactorily and/or on a timely basis. Both of these occurrences
would be beyond our control. We anticipate that we will similarly rely on
contract manufacturers for our future proprietary product candidates.
We
expect
to similarly rely on contract manufacturing relationships for any products
that
we may in-license or acquire in the future. However, there can be no assurance
that we will be able to successfully contract with such manufacturers on terms
acceptable to us, or at all.
Contract
manufacturers are subject to ongoing periodic inspections by the FDA, the U.S.
Drug Enforcement Agency and corresponding state agencies to ensure strict
compliance with cGMP and other state and federal regulations. Our contractor
in
Israel faces similar inspections from Israeli regulatory agencies and from
the
FDA. We do not have control over third-party manufacturers’ compliance with
these regulations and standards, other than through contractual obligations.
If
we
need to change manufacturers, the FDA and corresponding foreign regulatory
agencies must approve these new manufacturers in advance, which will involve
testing and additional inspections to ensure compliance with FDA regulations
and
standards and may require significant lead times and delay. Furthermore,
switching manufacturers may be difficult because the number of potential
manufacturers is limited. It may be difficult or impossible for us to find
a
replacement manufacturer quickly or on terms acceptable to us, or at
all.
Government
and Industry Regulation
Numerous
governmental authorities, principally the FDA and corresponding state and
foreign regulatory agencies, impose substantial regulations upon the clinical
development, manufacture and marketing of our drug candidates and technologies,
as well as our ongoing research and development activities. None of our drug
candidates have been approved for sale in any market in which we have marketing
rights. Before marketing in the United States, any drug that we develop must
undergo rigorous pre-clinical testing and clinical trials and an extensive
regulatory approval process implemented by the FDA, under the Federal Food,
Drug
and Cosmetic Act
of 1938,
as amended.
The FDA
regulates, among other things, the pre-clinical and clinical testing, safety,
efficacy, approval, manufacturing, record keeping, adverse event reporting,
packaging, labeling, storage, advertising, promotion, export, sale and
distribution of biopharmaceutical products.
The
regulatory review and approval process is lengthy, expensive and uncertain.
We
are required to submit extensive pre-clinical and clinical data and supporting
information to the FDA for each indication or use to establish a drug
candidate’s safety and efficacy before we can secure FDA approval. The approval
process takes many years, requires the expenditure of substantial resources
and
may involve ongoing requirements for post-marketing studies or surveillance.
Before commencing clinical trials in humans, we must submit an IND to the FDA
containing, among other things, pre-clinical data, chemistry, manufacturing
and
control information, and an investigative plan. Our submission of an IND may
not
result in FDA authorization to commence a clinical trial.
The
FDA
may permit expedited development, evaluation, and marketing of new therapies
intended to treat persons with serious or life-threatening conditions for which
there is an unmet medical need under its fast track drug development programs.
A
sponsor can apply for fast track designation at the time of submission of an
IND, or at any time prior to receiving marketing approval of the new drug
application, or NDA. To receive fast track designation, an applicant must
demonstrate that the drug:
|
·
|
is
intended to treat a serious or life-threatening
condition;
|
|
·
|
is
intended to treat a serious aspect of the condition;
and
|
|
·
|
has
the potential to address unmet medical needs, and this potential
is being
evaluated in the planned drug development
program.
|
Clinical
testing must meet requirements for institutional review board oversight,
informed consent and good clinical practices, and must be conducted pursuant
to
an IND, unless exempted.
The
FDA
must respond to a request for fast track designation within 60 calendar days
of
receipt of the request. Over the course of drug development, a product in a
fast
track development program must continue to meet the criteria for fast track
designation. Sponsors of products in fast track drug development programs must
be in regular contact with the reviewing division of the FDA to ensure that
the
evidence necessary to support marketing approval will be developed and presented
in a format conducive to an efficient review. Sponsors of products in fast
track
drug development programs ordinarily are eligible for priority review and also
may be permitted to submit portions of an NDA to the FDA for review before
the
complete application is submitted.
For
purposes of NDA approval, clinical trials are typically conducted in the
following sequential phases:
|
·
|
Phase
I:
The drug is administered to a small group of humans, either healthy
volunteers or patients, to test for safety, dosage tolerance, absorption,
metabolism, excretion, and clinical pharmacology.
|
|
·
|
Phase
II:
Studies are conducted on a larger number of patients to assess the
efficacy of the product, to ascertain dose tolerance and the optimal
dose
range, and to gather additional data relating to safety and potential
adverse events.
|
|
·
|
Phase
III:
Studies establish safety and efficacy in an expanded patient population.
|
|
·
|
Phase
IV:
The FDA may require a Phase IV to conduct post-marketing studies
for
purposes of gathering additional evidence of safety and
efficacy.
|
The
length of time necessary to complete clinical trials varies significantly and
may be difficult to predict. Clinical results are frequently susceptible to
varying interpretations that may delay, limit or prevent regulatory approvals.
Additional factors that can cause delay or termination of our clinical trials,
or that may increase the costs of these trials, include:
|
·
|
slow
patient enrollment due to the nature of the clinical trial plan,
the
proximity of patients to clinical sites, the eligibility criteria
for
participation in the study or other factors;
|
|
·
|
inadequately
trained or insufficient personnel at the study site to assist in
overseeing and monitoring clinical trials or delays in approvals
from a
study site’s review board;
|
|
·
|
longer
treatment time required to demonstrate efficacy or determine the
appropriate product dose;
|
|
·
|
insufficient
supply of the drug candidates;
|
|
·
|
adverse
medical events or side effects in treated patients; and
|
|
·
|
ineffectiveness
of the drug candidates.
|
In
addition, the FDA may place a clinical trial on hold or terminate it if it
concludes that subjects are being exposed to an unacceptable health risk. Any
drug is likely to produce some toxicity or undesirable side effects in animals
and in humans when administered at sufficiently high doses and/or for a
sufficiently long period of time. Unacceptable toxicity or side effects may
occur at any dose level at any time in the course of studies in animals designed
to identify unacceptable effects of a drug candidate, known as toxicological
studies, or clinical trials of drug candidates. The appearance of any
unacceptable toxicity or side effect could cause us or regulatory authorities
to
interrupt, limit, delay or abort the development of any of our drug candidates
and could ultimately prevent approval by the FDA or foreign regulatory
authorities for any or all targeted indications.
Before
receiving FDA approval to market a product, we must demonstrate that the product
is safe and effective for its intended use by submitting to the FDA an NDA
containing the pre-clinical and clinical data that have been accumulated,
together with chemistry and manufacturing and controls specifications and
information, and proposed labeling, among other things. The FDA may refuse
to
accept an NDA for filing if certain content criteria are not met and, even
after
accepting an NDA, the FDA may often require additional information, including
clinical data, before approval of marketing a product.
As
part
of the approval process, the FDA must inspect and approve each manufacturing
facility. Among the conditions of approval is the requirement that a
manufacturer’s quality control and manufacturing procedures conform to cGMP.
Manufacturers must expend time, money and effort to ensure compliance with
cGMP,
and the FDA conducts periodic inspections to certify compliance. It may be
difficult for our manufacturers or us to comply with the applicable cGMP and
other FDA regulatory requirements. If we or our contract manufacturers fail
to
comply, then the FDA will not allow us to market products that have been
affected by the failure.
If
the
FDA grants approval, the approval will be limited to those disease states,
conditions and patient populations for which the product is safe and effective,
as demonstrated through clinical studies. Further, a product may be marketed
only in those dosage forms and for those indications approved in the NDA.
Certain changes to an approved NDA, including, with certain exceptions, any
changes to labeling, require approval of a supplemental application before
the
drug may be marketed as changed. Any products that we manufacture or distribute
pursuant to FDA approvals are subject to continuing regulation by the FDA,
including compliance with cGMP and the reporting of adverse experiences with
the
drugs. The nature of marketing claims that the FDA will permit us to make in
the
labeling and advertising of our products will be limited to those specified
in
an FDA approval, and the advertising of our products will be subject to
comprehensive regulation by the FDA. Claims exceeding those that are approved
will constitute a violation of the Federal Food, Drug, and Cosmetic Act.
Violations of the Federal Food, Drug, and Cosmetic Act or regulatory
requirements at any time during the product development process, approval
process, or after approval may result in agency enforcement actions, including
withdrawal of approval, recall, seizure of products, injunctions, fines and/or
civil or criminal penalties. Any agency enforcement action could have a material
adverse effect on our business.
Should
we
wish to market our products outside the U.S., we must receive marketing
authorization from the appropriate regulatory authorities. The requirements
governing the conduct of clinical trials, marketing authorization, pricing
and
reimbursement vary widely from country to country. At present, companies are
typically required to apply for foreign marketing authorizations at a national
level. However, within the E.U., registration procedures are available to
companies wishing to market a product in more than one E.U. member state. If
the
regulatory authority is satisfied that a company has presented adequate evidence
of safety, quality and efficacy, the regulatory authority will grant a marketing
authorization. This foreign regulatory approval process involves all of the
risks associated with FDA approval discussed above. Our current strategy does
call for us to market our drug candidates outside the U.S.
Failure
to comply with applicable federal, state and foreign laws and regulations would
likely have a material adverse effect on our business. In addition, federal,
state and foreign laws and regulations regarding the manufacture and sale of
new
drugs are subject to future changes. We cannot predict the likelihood, nature,
effect or extent of adverse governmental regulation that might arise from future
legislative or administrative action, either in the U.S. or abroad.
Organizational
structure
Our
wholly-owned subsidiary, XTL Biopharmaceuticals, Inc., is incorporated in
Delaware and has its principal place of business in New York, New York.
Property,
Plant and Equipment
We
lease
an aggregate of approximately 1,870 square meters of office and laboratory
facilities in Rehovot, Israel. The lease in Rehovot expires in December 2006,
with an option to extend for an additional year through December 31, 2007.
We
currently lease approximately 2,790 square meters in Valley Cottage, New York,
and 55 square meters in Durham, North Carolina. The leases in Valley Cottage
and
Durham expire in 2009, and in October 2006, respectively. We have an option
to
renew our lease agreements, as needed. We also lease an approximate 100 square
meter area in New York, New York, which is subject to a rent sharing agreement
with the lessee of the facility.
We
anticipate that these facilities will be sufficient for our needs for the
foreseeable future. To our knowledge, there are no environmental issues that
affect our use of the properties that we lease.
There
are
no encumbrances on our rights in these leased properties or on any of the
equipment that we own. However, to
secure
the lease agreements in Israel, we provided a bank guarantee. As of December
31,
2005, the guarantee is secured by pledge on a long-term deposit amounting to
$110,000 linked to the Israeli Consumer Price Index, which is included in the
balance sheet as a restricted long-term deposit.
Material
Contracts
Yeda
License Agreement
In
April
of 1993, we entered into a research and license agreement with Yeda, which
we
refer to as the Yeda Agreement, under which Yeda granted us an exclusive
worldwide license to use the Trimera patent portfolio and to exclusively use
the
information derived from the performance of certain research for the purposes
specified in the agreement in any country where a licensed patent covers a
product sold under the license or other licensed activity until the date on
which the last licensed patent expires or until 12 years from the later of
the
first commercial sale of a product (or first receipts to us from other licensed
activity) in such country, and in any other country until 12 years from the
first commercial sale of a product (or first receipts to us from other licensed
activity) in that country. Under the agreement, any assignment of the license
granted by Yeda requires Yeda's prior written consent.
The
Yeda
Agreement has undergone a number of amendments, one of the end results of which
is that we shall pay to Yeda the following fees: a royalty of 3% of all net
sales received by us; 25% of amounts received by us on net sales of third
parties (less certain royalties payable by us to third parties), but no more
than 3% and no less than 1.5% of such net sales; and a royalty ranging between
20% to 40% on any receipts to us other than our net sales or receipts on net
sales made by third parties. Furthermore, such amendments have also changed
the
termination provisions relating to Yeda’s entitlement to terminate the agreement
if we do not pay Yeda a certain minimum amount of annual royalties of $100,000
or $200,000, depending on the year. We may terminate the agreement with Yeda
with six months advance notice in which event our rights in any technology
licensed by Yeda to us shall terminate and any technology derived from research
and development activities performed by us in connection with the technology
licensed by Yeda to us shall vest in Yeda.
In
the
most recent amendment of the Yeda Agreement, in order to facilitate the grant
of
the license by us to Cubist under the terms of the HepeX-B collaboration, Yeda
received the right to receive at least 1.5% of net sales of HepeX-B by Cubist
sub-licensees, regardless of the amount received by us from Cubist in respect
of
such sales.
Cubist
Collaboration
We
have
entered into a licensing agreement with Cubist dated June 2, 2004, as amended,
under which we granted to Cubist an exclusive, worldwide license (with the
right
to sub-license) to commercialize HepeX-B and any other product containing a
hMAb
or humanized monoclonal antibody or fragment directed at the hepatitis B virus
owned or controlled by us. Under this agreement, we were responsible for certain
clinical and product development activities of HepeX-B through August 2005,
at
the expense of Cubist. We have transferred full responsibility for completing
the development of HepeX-B to Cubist. Cubist will be responsible for completing
the development and for registration and commercialization of the product
worldwide. Nevertheless, during the term of this agreement, we have an ongoing
obligation to transfer to Cubist all information Cubist may reasonably require
and to provide Cubist with reasonable access to pertinent employees of ours
that
have experience with or information related to HepeX-B. We are also required
to
file, prosecute and maintain the relevant patents at our sole
expense.
In
the
event that the actual costs incurred in conducting activities that Cubist
determines are necessary or advisable to obtain regulatory approval for HepeX-B
for the prevention of recurrent hepatitis B infections in liver transplant
patients exceed $33.9 million, any costs in excess shall be borne in equal
share
by us and Cubist.
Under
the
terms of the agreement, Cubist paid us an initial up-front payment of $1 million
upon the signing of the agreement, a further aggregate amount of $1 million
was
paid in 2004, and an additional amount of up to $3 million will be paid upon
achievement of certain regulatory milestones. We are entitled to receive
royalties from net sales by Cubist, generally ranging from 10% to 17%, depending
on levels of net sales achieved by Cubist, subject to certain deductions based
on patent protection of HepeX-B in that territory, total costs of HepeX-B
development, third party license payments and indemnification
obligations.
Cubist
has the right to sub-license HepeX-B. The sub-licensee fees we will receive
in
such cases will vary according to the territory, the subject of the sub-license,
the patent protection of HepeX-B in that territory, total costs of HepeX-B
development, third party license payments, indemnification obligations and
local
competition. For example, where HepeX-B is not patent protected and a competing
product obtains more than an agreed percentage of the local market, we would
receive no royalties on sales of HepeX-B.
Cubist
has granted us the non-exclusive right of negotiation during the term of the
agreement to obtain all or any portion of the rights to manufacture and supply
HepeX-B or any other product containing an hMAb or humanized monoclonal antibody
or fragment directed at the hepatitis B virus owned or controlled by us.
Furthermore, in certain circumstances, we have the exclusive right to negotiate
with Cubist to obtain from Cubist a sub-license to market and sell the HepeX-B
or such other product in certain territories.
We
agreed
that during the term of the agreement and for one year thereafter, we will
not
research, develop or commercialize any competitive product containing a human
or
humanized monoclonal antibody or fragment that is directed to and binds with
the
hepatitis B virus.
The
agreement expires on the later of the last valid patent claim covering HepeX-B
to expire or 10 years after the first commercial sale of HepeX-B on a
country-by-country basis.
DRK-Blutspendedienst
Baden-Wurttemberg (Ulm University, Germany)
In
April
2000, we licensed Ab68 under an exclusive worldwide license from the
DRK-Blutspendedienst Baden-Wurttemberg (Ulm University, Germany, or Ulm). Under
the terms of this agreement, we are obligated to pay Ulm a specified royalty
rate on sales of product incorporating Ab68. We can deduct certain payments
that
are made to third parties from these royalties, subject to a minimum royalty
rate. We are also obligated to pay Ulm a specified percentage of any milestone
payments we may receive from any sublicensee to whom we may grant a license
or
sublicense of Ab68 or technology related to the production of Ab68. We can
deduct certain of these payments that are made to third parties from the
percentage of milestone payments owed to Ulm, subject to a minimum milestone
payment amount. Either party may terminate the agreement, by written notice,
upon or after the winding up or insolvency of the other party, or upon or after
commitment of a material breach by the other party that cannot be cured, or
if
curable, has not been cured, within 60 days after receipt of notice. In the
absence of such termination, the agreement shall expire upon the expiration
of
the license granted under the agreement. To date we have made $150,000 in
license and milestone payments to Ulm.
Stanford
University
In
September 2003, we licensed Ab65 from Stanford University under an exclusive
license agreement. Under the terms of this agreement, we have exclusive rights
to Ab65 worldwide, excluding China. In China, we have co-exclusive rights with
Applied Immunogenetics LLC. Under the terms of this agreement, we must use
commercially reasonable efforts to commercialize and market Ab65. We are
obligated to make royalty payments to Stanford University on sales of product
incorporating Ab65, and we are also obligated to make milestone payments upon
the occurrence of certain specified events. To date we have made $182,000 in
license and milestone payments to Stanford University, and we have undertaken
to
make contingent milestone payments of up to approximately $200,000 over the
life
of the license, all of which will be due upon or following regulatory approval
of the drug. The license terminates upon the later of the expiration of last
of
the licensed patents or at the time of our last royalty payment. Notwithstanding
the above, we may terminate this agreement upon specified notice to Stanford
University. In addition, should we fail to meet certain developmental milestones
for Ab65, our rights to the use of Ab65 become non-exclusive upon notice to
that
effect to us by Stanford University.
In
addition, as per an agreement entered into in September 2003, we are obligated
to make royalty payments on sales of product incorporating Ab65 to Applied
Immunogenetics LLC, a company that previously held non-exclusive rights to
Ab65
and returned them to Stanford University, enabling us to gain exclusive rights
to Ab65 from Stanford University. Our agreement with Applied Immunogenetics
LLC
expires on the expiration or termination of our exclusive agreement with
Stanford University, as described above. To date we have made $183,000 in
license and milestone payments to Applied Immunogenetics LLC. There are no
additional contingent milestone payments.
B&C
Biopharm Co., Ltd.
XTL-2125
has been licensed from B&C, since February 2003. Under the terms of the
agreement, we have exclusive rights to XTL-2125 worldwide, with the exception
of
Asia, which is shared between the two companies, and Korea, for which B&C
retains exclusive rights. Under the terms of the agreement, we are obligated
to
make certain milestone payments in addition to royalties on product sales.
To
date we have made $1.1 million in license and milestone payments to B&C, and
we have undertaken to make contingent milestone payments of up to approximately
$13.4 million over the life of the license, of which $8.0 million will be due
upon or following regulatory approval of the drug. The license terminates upon
the expiration of the last of the licensed patents. Notwithstanding the above,
we may terminate this agreement upon specified notice to B&C.
VivoQuest
Inc.
In
August
2005, we entered into an asset purchase agreement with VivoQuest, a privately
held biotechnology company based in the U.S., pursuant to which we agreed to
purchase from VivoQuest certain assets, including VivoQuest’s laboratory
equipment, and to assume VivoQuest’s lease of its laboratory space. In
consideration, we paid $450,000 to VivoQuest, which payment was satisfied by
the
issuance of ordinary shares having a fair market value in the same amount as
of
the closing date. In addition, we entered into a license agreement with
VivoQuest pursuant to which we acquired exclusive worldwide rights to
VivoQuest’s intellectual property and technology. The license covers a
proprietary compound library, including VivoQuest’s lead HCV compounds, that was
developed through the use of Diversity Oriented Synthesis, or DOS, technology.
The terms of the license agreement include an initial upfront license fee of
approximately $941,000 that was paid in our ordinary shares. The license
agreement also provides for additional milestone payments triggered by certain
regulatory and sales targets. These milestone payments total $34.6 million,
$25.0 million of which will be due upon or following regulatory approval or
actual product sales, and are payable in cash or ordinary shares at our
election. In addition, the license agreement requires that we make royalty
payments on product sales. The asset purchase agreement and the license
agreement with VivoQuest was completed in September 2005.
Directors
and Senior Management
The
following sets forth information with respect to our directors and executive
officers as of March 31, 2006. Except as noted, the business address for each
of
the following is 750 Lexington Avenue, 20th Floor, New York, New
York 10022.
|
Name
|
Age
|
Position
|
||
|
Michael
S. Weiss
|
40
|
Chairman
of the Board of Directors
|
||
|
William
J. Kennedy, Ph.D
|
61
|
Non
Executive Director
|
||
|
Ido
Seltenreich (1)
|
34
|
Non
Executive and External Director
|
||
|
Vered
Shany, D.M.D (1)
|
41
|
Non
Executive and External Director
|
||
|
Jonathan
R. Spicehandler, M.D
|
57
|
Non
Executive Director
|
||
|
Ben
Zion Weiner, Ph.D (1)
|
61
|
Non
Executive Director
|
||
|
Ron
Bentsur
|
40
|
Chief
Executive Officer
|
||
|
Jonathan
Burgin (1)
|
44
|
Chief
Financial Officer
|
(1)
Business
address is Kiryat
Weizmann Science Park, Building 3, POB 370, Rehovot 76100,
Isreal.
Michael
S. Weiss has served as a director of our company since November 2004, and was
appointed interim Chairman of the Board in March 2005 and Chairman of the Board
in August 2005. Mr. Weiss is currently the Chairman and CEO of Keryx
Biopharmaceuticals, Inc. (Nasdaq: KERX). Prior to that, from 1999-2002, Mr.
Weiss was the founder, chairman and CEO of ACCESS Oncology, Inc., a private
cancer company subsequently acquired by Keryx. Prior to that, Mr. Weiss was
Senior Managing Director at Paramount Capital, Inc. From 1991-1993, Mr. Weiss
was an attorney at Cravath, Swaine & Moore. Mr. Weiss received his B.A.,
magna cum laude from State University of New York at Albany and was awarded
a
Juris Doctorate degree from Columbia University Law School.
William
J. Kennedy has served as a director of our company since February 2005. Dr.
Kennedy retired as Vice President, Drug Regulatory Affairs, for Zeneca
Pharmaceuticals Group in October 1999, and since that time has served as a
regulatory consultant to the pharmaceutical industry. Prior to joining Zeneca
Pharmaceuticals in 1986, Dr. Kennedy worked in regulatory affairs at G.D. Searle
& Co., Kalipharma Inc., Berlex Laboratories, Inc. and Pfizer
Pharmaceuticals, Inc. Dr. Kennedy earned a B.S. from Siena College, a M.A.
from
Clark University and a Ph.D in Pharmacology from SUNY, Buffalo. Prior to joining
the industry in 1977, he was an Associate Research Professor at Yale University
conducting research in Molecular Biology and Recombinant DNA.
Ido
Seltenreich has served as a director of our company since August
2005.
Mr.
Seltenreich is currently the representative of Cinema City International N.V.,
or CCI, in the Czech Republic, for which he has served as the Managing and
Financing Director since October 1999.
Mr.
Seltenreich served as
a member
of the board of directors of an intragroup company of CCI, a development company
that operates in the Bulgarian market
from
July 2003 to August 2005.
Prior to
that, from 1996-1999, Mr. Seltenreich worked at Luboshits Kasirer, a member
of
Ernst & Young.
Mr.
Seltenreich received his B.A. in economics and accounting from Haifa University
and has an Israeli CPA license.
Vered
Shany has served as a director of our company since August 2005. Since March
2002, Dr. Shany has managed Tashik Consultants, providing strategic consulting
and corporate analysis for Israeli and international corporations and investment
management in life sciences companies. Previously, Dr. Shany served as managing
director of Up-Tech Ventures Ltd, a subsidiary of the Africa-Israel Investments
Group from May 2000 to March 2002, as a member of the board of directors of
the
Weizmann Science Park Incubator from May 2000 to March 2002, as vice president
of marketing for Arad Technological Incubator from 1995 to 1999 and as business
and marketing manager of Medun Ltd, a medical start-up company, from 1995 to
1998. Dr. Shany is currently an external director in Lahak Mutual Funds of
Bank
Hapoalim and in SFKT - Shrem Fudim Kellner Technologies. Dr. Shany received
her
masters’ degree in business administration from Heriot - Watt University,
Edinburgh Business School, completed her D.M.D. degree, Doctor of Medical
Dentistry and her B.Med.Sc, from Hebrew University of Jerusalem.
Jonathan
R. Spicehandler has served as a director of our company since February 2005.
Dr.
Spicehandler is the chairman of Schering-Plough Research Institute, the
pharmaceutical research arm of Schering-Plough Corporation, a research-based
company engaged in the discovery, development, manufacturing and marketing
of
pharmaceutical and health care products worldwide. Dr. Spicehandler assumed
his
present position in March 2002. He serves as a scientific advisor to the
Schering-Plough Operating Committee as well as to senior management. He joined
the company in 1982 as senior director - immunology and anti-infective clinical
research and was appointed Vice President - clinical research in 1985; Vice
President - biological research in 1991; Vice President - operations in 1992;
and became President, Schering-Plough Research Institute in 1993. Dr.
Spicehandler received his B.A. in biology from Union College in New York and
his
M.D. degree, cum laude, from the St. Louis University School of Medicine. Dr.
Spicehandler is also on the Board of Directors of Keryx Biopharmaceuticals,
Inc.
Ben
Zion
Weiner has served as a director of our company since February 2005. Dr. Weiner
has been with Teva Pharmaceutical Industries Ltd. since 1975, after a Post
Doctorate fellowship at Schering-Plough in the U.S.A. He received his Ph.D
in
Chemistry from the Hebrew University of Jerusalem. Since 2002 he has been Group
Vice President, Global Products at Teva, responsible for Global Generic Research
and Development, Global Innovative Research and Development and innovative
products marketing. Dr. Weiner is a member of Teva's Core Management Committee.
He was granted twice the Rothschild Prize for Innovation/Export, in 1989 for
the
development of alpha D3 for Dialysis and Osteoporosis and in 1999 for the
development of Copaxone® for Multiple Sclerosis.
Ron
Bentsur has served as our Chief Executive Officer since January 2006. Mr.
Bentsur has nearly a decade of experience in the biotech industry. From June
2003 until February 2006, Mr. Bentsur served as Vice President, Finance and
Investor Relations of Keryx Biopharmaceuticals, Inc. From October 2000 to June
2003, Mr. Bentsur served as Director of Investor Relations at Keryx. From July
1998 to October 2000, he served as Director of Technology Investment Banking
at
Leumi Underwriters, where he was responsible for all technology/biotechnology
private placement and advisory transactions. From June 1994 to July 1998, Mr.
Bentsur worked as an investment banker at ING Barings Furman Selz. Mr. Bentsur
holds a B.A. in Economics and Business Administration with distinction from
the
Hebrew University of Jerusalem, Israel and an M.B.A., Magna Cum Laude, from
New
York University’s Stern Graduate School of Business.
Jonathan
Burgin is a C.P.A. and has served as our Chief Financial Officer since August
1999. Before joining our company, he was the Chief Financial Officer at YLR
Capital Markets, a leading Israeli investment bank which was publicly traded
on
the Tel Aviv Stock Exchange. From 1984 to 1997, Mr. Burgin worked at Kesselman
& Kesselman, an accounting firm and a member of PricewaterhouseCoopers
International Limited. During the last three years of his tenure there, Mr.
Burgin served as Senior Manager. He received both his M.B.A. and B.A. in
accounting and economics from Tel Aviv University.
Employment
Agreements
We
have
an employment agreement dated as
of
January 3, 2006, with Ron Bentsur, Chief Executive Officer. Mr. Bentsur is
entitled to an annual base salary of $225,000. He is entitled to receive a
one
time bonus of $25,000 in the event we are successful in securing an equity
financing in excess of $10 million. He is entitled to receive discretionary
bonus payments of up to 100% of his annual base salary on achievement of certain
milestones recommended by the Remuneration Committee and set by our Board of
Directors. Mr. Bentsur was also granted options to purchase a total of 7,000,000
ordinary shares at an exercise price equal to $0.774 per share (closing price
of
the last trading day prior to official appointment). These options are
exercisable for a period of ten years from the date of issuance, and granted
under the same terms and conditions as the Share Option Plan 2001 (see “Share
Ownership - Share Option Plans” below) and any option agreement entered into
with Mr. Bentsur. Of these, 2,333,334 options shall vest as follows: 777,782
options on the one-year anniversary of the issuance of the options and 194,444
options at the end of each quarter thereafter for the following two years.
The
balance of options shall vest upon achievement of certain milestones (2,333,333
upon the achievement of $350 million market capitalization or $75 million in
working capital, as set out in the agreement and 2,333,333 upon the achievement
of $550 million market capitalization or $125 million in working capital, as
set
out in the agreement). We may terminate the agreement without cause (as defined
in the agreement) on 30 days’ prior notice to Mr. Bentsur, and immediately and
without prior notice for cause. Mr. Bentsur may terminate the agreement with
good reason (as defined in the agreement) on 30 days’ prior notice to us. In
addition, in the event of a merger, acquisition or other change of control
or in
the event that we terminate Mr. Bentsur, either without cause or as a result
of
his death or disability, or Mr. Bentsur terminates his agreement for good
reason, any outstanding but unvested options granted to Mr. Bentsur under the
agreement will immediately vest and the period during which he may exercise
such
options shall be the earlier of two years from the effective date of his
termination or ten years from the date he commenced employment. Additionally,
our board of directors shall have the discretion to accelerate all or a portion
of Mr. Bentsur’s options at any time. If we choose to terminate the agreement
for cause, Mr. Bentsur will not be owed any benefits, with the exception of
any
unpaid remuneration that would have accrued up to his date of
termination.
We
have
an employment agreement dated August 1, 1999, as amended, with Jonathan Burgin,
our Chief Financial Officer. Mr. Burgin is entitled to an annual base salary
of
$140,000. He is entitled to receive discretionary bonus payments of up to 25%
of
his annual base salary on achievement of certain milestones recommended by
the
Remuneration Committee and set by our Board of Directors. Mr. Burgin is also
entitled to receive benefits comprised of managers' insurance (pension and
disability insurance), a continuing education plan, and the use of a company
car. There is a non-compete clause surviving one year after termination of
employment, preventing Mr. Burgin from competing directly or indirectly with
us,
or soliciting our employees or customers. The employment agreement may be
terminated by either party on 14 days prior notice to the other, and in such
event, Mr. Burgin is entitled to an additional six months'
salary.
We
have
an agreement dated August 1, 2005, with Michael S. Weiss, our non-Executive
Chairman of the Board of Directors. Mr. Weiss is entitled to annual remuneration
of $150,000. He was granted options to purchase a total of 9,250,000 ordinary
shares at an exercise price equal to $0.354 per share. These options are
exercisable for a period of five years from the date of issuance, and granted
under the same terms and conditions as our 2001 Share Option Plan (see “Share
Ownership - Share Option Plans” below) and any option agreement that we may
enter into with Mr. Weiss. The options shall vest upon achievement of certain
market capitalization based milestones. We may terminate the agreement without
cause (as defined in the agreement) on 30 days’ prior notice to Mr. Weiss, and
immediately and without prior notice for cause. Mr. Weiss may terminate the
agreement with good reason (as defined in the agreement) on 30 days prior notice
to us. In the event that the agreement is terminated without cause (in our
case)
or with good reason (in the case of Mr. Weiss), any outstanding but unvested
options granted to Mr. Weiss under the agreement will immediately vest and
the
period during which he may exercise such options will be extended. If we choose
to terminate the agreement for cause, Mr. Weiss will not be owed any benefits,
with the exception of any unpaid remuneration that would have accrued through
his date of termination. In addition, in March 2006, the audit committee and
the
Board of Directors approved the grant of 9,898,719 options to Mr. Weiss. This
option grant is subject to approval by our shareholders, see details under
“Compensation” below.
We
have
three types of service agreements with our directors, other than our agreement
with our non-Executive Chairman. The first type, entered into with Ben Zion
Weiner, provides for a grant of 2,000,000 options having an exercise price
equal
to $0.354 per share, exercisable for a period of five years and vesting upon
achievement of certain market capitalization based milestones. The second type
of director service agreement, entered into with William Kennedy and Jonathan
Spicehandler, provides for a grant of 60,000 options having an exercise price
equal $0.853, vesting over the three years from the date of grant. In addition,
the second type of director service agreement provides for three annual grants
of 20,000 options each, at an exercise price equivalent to the then current
closing price of our ADRs on the Nasdaq Stock Market (subject to the ordinary
share-ADR ratio). The third type, entered into with Ido Seltenreich and Vered
Shany, does not provide for option grants, and has a term of 36 months, unless
terminated by the director upon two months’ written notice to us. Each of the
three types of director service agreements provides for an annual salary of
$20,000, payments of $2,000 for attendance at each board meeting and $500 for
attendance at each committee meeting, reimbursement of reasonable out-of-pocket
expenses, and termination by the director on two months’ written notice to us.
In addition, in March 2006, the Audit Committee and the Board of Directors
approved the grant of a total of 750,000 options to Mr. Weiner. This option
grant is subject to approval by our shareholders, see details under
“Compensation” below.
Compensation
The
aggregate compensation paid by us and by our wholly-owned subsidiary to all
persons who served as directors or senior management for the year 2005 (10
persons) was approximately $0.6 million. This amount includes payments made
for
social security, pension and disability insurance premiums of approximately
$0.1
million, as well as payments made in lieu of statutory severance, payments
for
continuing education plans, payments made for the redemption of accrued
vacation, and amounts expended by us for automobiles made available to our
officers.
During
2005, we granted a total of 11,250,000 options to our Chairman and one of our
non-executive directors. These options are exercisable at $0.354 per ordinary
share, and expire five years after their respective date of grant. In addition,
we granted a total of 120,000 options to two of our non-executive directors.
These options are exercisable at $0.853 per ordinary share, and expire ten
years
after their respective date of grant.
In
March
2006, our board of directors granted our Chief Executive Officer options to
purchase a total of 7,000,000 ordinary shares at an exercise price equal to
$0.774 per share (closing price of the last trading day prior to official
appointment). These options are exercisable for a period of ten years from
the
date of issuance, and granted under the same terms and conditions as the Share
Option Plan 2001 (see “Share Ownership - Share Option Plans” below) and any
option agreement entered into with Mr. Bentsur. Of these, 2,333,334 options
shall vest as follows: 777,782 options on the one-year anniversary of the
issuance of the options and 194,444 options at the end of each quarter
thereafter for the following two years. The balance of options shall vest upon
achievement of certain milestones (2,333,333 upon the achievement of $350
million market capitalization or $75 million in working capital, as set out
in
the agreement and 2,333,333 upon the achievement of $550 million market
capitalization or $125 million in working capital, as set out in the
agreement).
In
March
2006, the board of directors also approved grants of a total of 9,898,719
options to our Chairman and 750,000 options to one of our non-executive
directors. These options are exercisable at an exercise price which is the
volume weighted average price per share of the ADRs on Nasdaq during the thirty
trading days prior to the board of directors’ approval divided by ten, $0.713.
The options shall vest as follows: (i) 1/3 of such options shall vest over
three
years, of which amounts, 1/3 shall vest and be exercisable upon the first
anniversary of the issuance of the options and the remainder shall vest and
be
exercisable on a quarterly basis; (ii) 1/3 of such options shall vest and be
exercisable upon our achieving a total market capitalization on a fully diluted
basis of more than US $350 million; and (iii) 1/3 of such options shall vest
upon our achieving a total market capitalization on a fully diluted basis of
more than US $550 million. The options can be exercised for a period of ten
years. The grant of such options is conditional upon approval of the
shareholders at a duly convened shareholder meeting expected to take place
later
this year.
All
members of our board of directors who are not our employees are reimbursed
for
their expenses for each meeting attended. Our directors who are not external
directors as defined by the Israeli Companies
Act
are
eligible to receive share options under our share option plans. Non-executive
directors do not receive any remuneration from us other than their fees for
services as members of the board, additional fees if they serve on committees
of
the board and expense reimbursement.
In
accordance with the requirements of Israeli Law, we determine our directors’
compensation in the following manner:
|
·
|
first,
our audit committee reviews the proposal for
compensation;
|
|
·
|
second,
provided that the audit committee approves the proposed compensation,
the
proposal is then submitted to our board of directors for review,
except
that a director who is the beneficiary of the proposed compensation
does
not participate in any discussion or voting with respect to such
proposal;
and
|
|
·
|
finally,
if our board of directors approves the proposal, it must then submit
its
recommendation to our shareholders, which is usually done in connection
with our shareholders’ general
meeting.
|
The
approval of a majority of the shareholders voting at a duly convened
shareholders meeting is required to implement any such compensation
proposal.
Board
practices
Election
of Directors and Terms of Office
Our
board
of directors currently consists of six members, including our chairman. Other
than our two external directors, our new directors are elected by an ordinary
resolution at the annual general meeting of our shareholders. The nomination
of
our directors is proposed by a nomination committee of our board of directors,
whose proposal is then approved by the board. The current members of the
nomination committee are Jonathan Spicehandler (chairman of the nomination
committee), Ido Seltenreich and Vered Shany. Our board, following receipt of
a
proposal of the nomination committee, has the authority to add additional
directors up to the maximum number of 12 directors allowed under the Articles.
Such directors appointed by the board serve until the next annual general
meeting of the shareholders in which their term of office shall expire. In
August 2005, at the annual general meeting of our shareholders, Michael Weiss,
Ben Zion Weiner, William Kennedy and Jonathan Spicehandler were re-elected
to
serve as directors of our company and Ido Seltenreich and Vered Shany were
elected to serve as external directors of our company. Unless they resign before
the end of their term or are removed in accordance with our Articles of
Association, all our directors, other than our external directors, will serve
as
directors until our next annual general meeting of shareholders.
Ido
Seltenreich and Vered Shany are serving as external directors pursuant to the
provisions of the Israeli Companies Law for a three-year term ending in August
2008, as more fully described below. After this date, their term of service
may
be renewed for an additional three-year term.
None
of
our directors or officers have any family relationship with any other director
or officer.
None
of
our directors are entitled to receive any severance or similar benefits upon
termination of his or her service, except for our chairman, as more fully
described above in “ - Employment Agreements.”
Our
Articles of Association permit us to maintain directors and officers’ liability
insurance and to indemnify our directors and officers for actions performed
on
behalf of us, subject to specified limitations. We maintain a directors and
officers insurance policy which covers the liability of our directors and
officers as allowed under Israeli Companies Law.
External
and Independent Directors
The
Israeli Companies Law requires Israeli companies with shares that have been
offered to the public either in or outside of Israel to appoint two external
directors. No person may be appointed as an external director if that person
or
that person’s relative, partner, employer or any entity under the person’s
control, has or had, on or within the two years preceding the date of that
person's appointment to serve as an external director, any affiliation with
the
company or any entity controlling, controlled by or under common control with
the company. The term affiliation includes:
|
·
|
an
employment relationship;
|
|
·
|
a
business or professional relationship maintained on a regular
basis;
|
|
·
|
control;
and
|
|
·
|
service
as an office holder, other than service as an officer for a period
of not
more than three months, during which the company first offered shares
to
the public.
|
No
person
may serve as an external director if that person’s position or business
activities create, or may create, a conflict of interest with that person's
responsibilities as an external director or may otherwise interfere with his/her
ability to serve as an external director. If, at the time external directors
are
to be appointed, all current members of the board of directors are of the same
gender, then at least one external director must be of the other gender. A
director in one company shall not be appointed as an external director in
another company if at that time a director of the other company serves as an
external director in the first company. In addition, no person may be appointed
as an external director if he/she is a member or employee of the Israeli
Security Authority, and also not if he/she is a member of the board of directors
or an employee of a stock exchange in Israel.
External
directors are to be elected by a majority vote at a shareholders' meeting,
provided that either:
|
·
|
the
majority of shares voted at the meeting, including at least one-third
of
the shares held by non-controlling shareholders voted at the meeting,
vote
in favor of election of the director, with abstaining votes not being
counted in this vote; or
|
|
·
|
the
total number of shares held by non-controlling shareholders voted
against
the election of the director does not exceed one percent of the aggregate
voting rights in the company.
|
The
initial term of an external director is three years and may be extended for
an
additional three-year term. External directors may be removed only by the same
percentage of shareholders as is required for their election, or by a court,
and
then only if the external directors cease to meet the statutory qualifications
for their appointment or if they violate their duty of loyalty to the company.
At least one external director must serve on every committee that is empowered
to exercise one of the functions of the board of directors.
An
external director is entitled to compensation as provided in regulations adopted
under the Israeli Companies Law and is otherwise prohibited from receiving
any
other compensation, directly or indirectly, in connection with service provided
as an external director.
Ido
Seltenreich and Vered Shany serve as external directors pursuant to the
provisions of the Israeli Companies Law and as our independent directors under
the corporate governance codes of practice requirements of the London Stock
Exchange. They both serve on our audit committee, our nomination committee
and
our compensation committee.
Subject
to certain exceptions, issuers that list on Nasdaq must have boards of directors
including a majority of independent directors, as such term is defined by
Nasdaq. In addition, both SEC and Nasdaq rules mandate that the audit committee
of a listed issuer consist of at least three members, all of whom must be
independent, as such term is defined by rules and regulations promulgated by
the
SEC. We are in compliance with the independence requirements of both the SEC
and
Nasdaq.
Audit
Committee
The
Israeli Companies Law requires public companies to appoint an audit committee.
The responsibilities of the audit committee include identifying irregularities
in the management of the company’s business and approving related party
transactions as required by law. An audit committee must consist of at least
three directors, including all of its external directors. The chairman of the
board of directors, any director employed by or otherwise providing services
to
the company, and a controlling shareholder or any relative of a controlling
shareholder, may not be a member of the audit committee. An audit committee
may
not approve an action or a transaction with a controlling shareholder, or with
an office holder, unless at the time of approval two external directors are
serving as members of the audit committee and at least one of the external
directors was present at the meeting in which an approval was granted.
Our
audit
committee is currently comprised of three independent non-executive directors.
The audit committee is chaired by Ido Seltenreich, who serves as the audit
committee financial expert, with William Kennedy and Vered Shany as members.
The
audit committee meets at least twice a year and monitors the adequacy of our
internal controls, accounting policies and financial reporting. It regularly
reviews the results of the ongoing risk self-assessment process, which we
undertake, and our interim and annual reports prior to their submission for
approval by the full board of directors. The audit committee oversees the
activities of the internal auditor, sets its annual tasks and goals and reviews
its reports. The audit committee reviews the objectivity and independence of
the
external auditors and also considers the scope of their work and fees. In
accordance with the Nasdaq requirements, our audit committee is directly
responsible for the appointment, compensation and oversight of our independent
auditors.
We
have
adopted a written charter for our audit committee, setting forth its
responsibilities as outlined by Nasdaq rules and the regulations of the SEC.
In
addition, our audit committee has adopted procedures for the receipt, retention
and treatment of complaints we may receive regarding accounting, internal
accounting controls, or auditing matters and the submission by our employees
of
concerns regarding questionable accounting or auditing matters.
Approval
of Compensation to Our Officers
The
Israeli Companies Law prescribes that compensation to officers must be approved
by a company's board of directors. Nasdaq corporate governance rules require
that compensation of the chief executive officer and other executive officers
be
determined, or recommended to the board of directors, by a majority of the
independent directors or by a compensation committee comprised solely of
independent directors. We have established a compensation committee in
compliance with the Israeli Companies Law and Nasdaq rules.
Our
compensation committee consists of three independent directors: Vered Shany
(chairman of the compensation committee), William Kennedy and Ido Seltenreich.
The responsibilities of the compensation committee are to set our overall policy
on executive remuneration and to decide the specific remuneration, benefits
and
terms of employment for each senior manager, including the Chief Executive
Officer.
The
objectives of the compensation committee’s policies are that senior managers
should receive compensation which is appropriate given their performance, level
of responsibility and experience. Compensation packages should also allow us
to
attract and retain executives of the necessary caliber while, at the same time,
motivating them to achieve the highest level of corporate performance in line
with the best interests of shareholders. In order to determine the elements
and
level of remuneration appropriate to each executive director, the compensation
committee reviews surveys on executive pay, obtains external professional advice
and considers individual performance.
Internal
Auditor
Under
the
Israeli Companies Law, the board of directors must appoint an internal auditor,
nominated by the audit committee. The role of the internal auditor is to
examine, among other matters, whether the company's actions comply with the
law
and orderly business procedure. Under the Israeli Companies Law, the internal
auditor cannot be an office holder, an interested party or a relative of an
office holder or interested party, and he or she may not be the company's
independent accountant or its representative. We comply with the requirement
of
the Israeli Companies Law relating to internal auditors. Our internal auditors
examine whether our various activities comply with the law and orderly business
procedure.
Compliance
with Nasdaq Corporate Governance Requirements
Under
the
Nasdaq corporate governance rules, foreign private issuers are exempt from
many
of the requirements if they instead elect to comply with home country practices
and disclose where they have elected to do so. As noted above, we are currently
in compliance with Nasdaq rules relating to the independence of our board of
directors and our audit committee. Our board of directors and our audit
committee have adopted a written charter for the audit committee setting forth
the responsibilities of the audit committee as required by the SEC and Nasdaq.
Also as noted above, we currently have a nomination committee to identify,
review and recommend to the Board of Directors individuals believed to be
qualified to become directors. We have adopted a written charter for the
nomination committee, as required by Nasdaq. We currently have in place a
compensation committee, as discussed in more detail above. We have adopted
a
written charter for the compensation committee.
In
August
2005, our board of directors adopted a Code of Conduct that applies to all
employees, directors and officers of our company, including our principal
executive officer, principal financial officer, principal accounting officer
or
controller and other individuals performing similar functions. A copy of our
Code of Conduct may be obtained, without charge, upon a written request
addressed to our investor relations department, XTL Biopharmaceuticals Ltd.,
750
Lexington Avenue, 20th
Floor,
New York, NY (telephone no. 212-531-5960).
Employees
As
of
March 31, 2006, we had 42 full-time employees. We and our Israeli employees
are
subject, by an extension order of the Israeli Ministry of Welfare, to a few
provisions of collective bargaining agreements between the Histadrut, the
General Federation of Labor Unions in Israel and the Coordination Bureau of
Economic Organizations, including the Industrialists Associations. These
provisions principally address cost of living increases, recreation pay, travel
expenses, vacation pay and other conditions of employment. We provide our
employees with benefits and working conditions equal to or above the required
minimum. Other than those provisions, our employees are not represented by
a
labor union. We have written employment contracts with our employees, and we
believe that our relations with our employees are good.
For
the
years ended December 31, 2005, 2004 and 2003, the number of our employees
engaged in the specified activities, by geographic location, are presented
in
the table below.
|
Year
ended December 31,
|
||||||||||
|
2005
|
2004
|
2003
|
||||||||
|
Research
and Development
|
||||||||||
|
Israel
|
22
|
44
|
42
|
|||||||
|
U.S
|
19
|
8
|
5
|
|||||||
|
41
|
52
|
47
|
||||||||
|
Financial
and general management
|
||||||||||
|
Israel
|
4
|
7
|
6
|
|||||||
|
U.S
|
--
|
--
|
--
|
|||||||
|
4
|
7
|
6
|
||||||||
|
Business
development
|
||||||||||
|
Israel
|
--
|
--
|
--
|
|||||||
|
U.S
|
1
|
1
|
2
|
|||||||
|
1
|
1
|
2
|
||||||||
|
Total
|
46
|
60
|
55
|
|||||||
|
Average
number of full-time employees
|
54
|
58
|
68
|
|||||||
Share
Ownership
Share
Ownership by Directors and Senior Management
The
following table sets forth certain information as of March 31, 2006, regarding
the beneficial ownership by our directors and executive officers. All numbers
quoted in the table are inclusive of options to purchase shares that are
exercisable within 60 days of March 31, 2006.
|
Amount
and nature of beneficial ownership
|
|||||||||||||
|
|
Ordinary
shares
beneficially
owned
excluding
options
|
Options
exercisable
within
60 days
of March 31,
2006
|
Total
ordinary
shares
beneficially
owned
|
Percent
of
ordinary
shares
beneficially
owned(1)
|
|||||||||
|
Michael
S. Weiss
Chairman
of the Board
|
--
|
3,083,333
|
3,083,333
|
1.75
|
%
|
||||||||
|
William
Kennedy
Director
|
--
|
--
|
--
|
--
|
|||||||||
|
Jonathan
Spicehandler
Director
|
--
|
--
|
--
|
--
|
|||||||||
|
Ben
Zion Weiner
Director
|
--
|
666,667
|
666,667
|
0.38
|
%
|
||||||||
|
Ido
Seltenreich
Director
|
250,000
|
--
|
250,000
|
0.14
|
%
|
||||||||
|
Vered
Shany
Director
|
--
|
--
|
--
|
--
|
|||||||||
|
Ron
Bentsur
Chief
Executive Officer
|
--
|
--
|
--
|
--
|
|||||||||
|
Jonathan
Burgin
Chief
Financial Officer
|
20,000
|
1,382,053
|
1,402,053
|
0.80
|
%
|
||||||||
|
All
directors and executive officers as a group
(8 persons)
|
270,000
|
5,132,053
|
5,402,053
|
3.03
|
%
|
||||||||
|
|
|
||||||||||||
(1)
Excludes the effects of the private placement that closed on March 22,
2006.
Share
Option Plans
We
maintain the following share option plans for our and our subsidiary’s
employees, directors and consultants. In addition to the discussion below,
see
Note 6 of our consolidated financial statements.
Our
board
of directors administers our share option plans and has the authority to
designate all terms of the options granted under our plans including the
grantees, exercise prices, grant dates, vesting schedules and expiration dates,
which may be no more than ten years after the grant date. Options may not be
granted with an exercise price of less than the fair market value of our
ordinary shares on the date of grant, unless otherwise determined by our board
of directors.
As
of
March 31, 2006, we have granted to employees, officers and directors and
consultants options that are outstanding to purchase up to 31,684,192 ordinary
shares, under the five share option plans and pursuant to certain grants apart
from these plans as discussed below.
1998
Share Option Plan
Under
a
share option plan established in 1998, we granted options to our employees
which
are held by a trustee under section 3(i) of the Tax Ordinance, of which
3,884,810 are outstanding at an exercise price per share of $0.497. The options
are non-transferable.
The
option term is for a period of 10 years from grant date. If the options are
not
exercised and the shares not paid for by such date, all interests and rights
of
any grantee shall expire. The options were granted for no consideration and
are
fully vested.
1999
Share Option Plan
Under
a
share option plan established in 1999, we granted options to our employees
which
are held by a trustee under section 3(i) of the Tax Ordinance, of which 940,020
are outstanding, at an exercise price of $0.497. The options are
non-transferable.
The
option term is for a period of 10 years from grant date. If the options are
not
exercised and the shares not paid for by such date, all interests and rights
of
any grantee shall expire. The options were granted for no consideration and
are
fully vested.
1999
International Share Option Plan
Under
an
international share option plan established in 1999, we granted options to
our
employees of which 1,380,000 are outstanding at an exercise price between $0.497
and $1.10. The options are non transferable.
The
options granted thereunder are outstanding and exercisable until October 2007.
If the options are not exercised and the shares are not paid for by such date,
all interests and rights of any grantee shall expire. The options were granted
for no consideration and are fully vested.
2000
Share Option Plan
Under
a
share option plan established in 2000, we granted options to our employees
which
are held by a trustee under section 3(i) of the Tax Ordinance, of which 855,300
are outstanding, at an exercise price of $1.10. The options are
non-transferable.
The
option term is for a period of 10 years from grant date. If the options are
not
exercised and the shares not paid for by such date, all interests and rights
of
any grantee shall expire. The options were granted for no consideration and
are
fully vested.
2001
Share Option Plan
Under
a
share option plan established in 2001, referred to as the 2001 Plan, we granted
options to our employees, including directors who are employees, of which
2,469,602 are outstanding at an exercise price per share between $0.106 and
$0.931. These options were granted in accordance with section 102 of the Tax
Ordinance, under the capital gains option set out in section 102(b)(2) of the
ordinance. The options are non-transferable.
The
option term is for a period of 10 years from grant date. The options were
granted for no consideration. All options vest on an annual basis over a period
of three years. As of March 31, 2006, 2,453,134 options were vested.
Non-Plan
Share Options
In
addition to the options granted under our share option plans, there are
21,974,460 outstanding options, as of March 31, 2006, which were granted by
our
board of directors to employees, directors and consultants not under an option
plan. The options were granted at an exercise price per share between $0.200
and
$2.110. The options expire between 2007 and 2016. This figure includes options
granted to consultants as in conjunction with a licensing agreement with
Stanford University to purchase a total of up to 320,000 of our ordinary shares
at an exercise price per share of $0.200. As of March 31, 2006, 7,184,460
options were vested.
In
August
2005, our shareholders granted Michael S. Weiss, the Chairman of the Board,
and
Ben Zion Weiner, a non-executive director, options to purchase a total of
9,250,000 and 2,000,000 ordinary shares, respectively, at an exercise price
equal to $0.354 per share. These options are exercisable for a period of five
years from the date of issuance, and granted under the same terms and conditions
as our 2001 Plan. The options shall vest upon achievement of certain market
capitalization based milestones recommended by the Audit Committee and set
by
our Board of Directors and approved by the shareholders at our annual
shareholders’ meeting in August 2005.
In
addition, in August 2005, our shareholders approved grants to William Kennedy
and Jonathan Spicehandler, each a non-executive director, of 60,000 options
each, having an exercise price equal to $0.853 per share, vesting over the
three
years from the date of grant, and furthermore approved three annual grants
of
20,000 options each, at an exercise price equivalent to the then current closing
price of our ADRs on the Nasdaq Stock Market (subject to the ordinary share-ADR
ratio).
In
March
2006, our board of directors granted our Chief Executive Officer options to
purchase a total of 7,000,000 ordinary shares at an exercise price equal to
$0.774 per share (closing price of the last trading day prior to official
appointment). These options are exercisable for a period of ten years from
the
date of issuance, and granted under the same terms and conditions as the 2001
Plan (see “Share Option Plans” above) and any option agreement entered into with
Mr. Bentsur. Of these, 2,333,334 options shall vest as follows: 777,782 options
on the one-year anniversary of the issuance of the options and 194,444 options
at the end of each quarter thereafter for the following two years. The balance
of options shall vest upon achievement of certain milestones (2,333,333 upon
the
achievement of $350 million market capitalization or $75 million in working
capital, as set out in the agreement and 2,333,333 upon the achievement of
$550
million market capitalization or $125 million in working capital, as set out
in
the agreement).
In
March
2006, the board of directors also approved grants of a total of 9,898,719
options to our Chairman and 750,000 options to one of our non-executive
directors. These options are exercisable at an exercise price which is the
volume weighted average price per share of the ADRs on NASDAQ during the thirty
trading days prior to the board of directors’ approval divided by ten, $0.713.
The options shall vest as follows: (i) 1/3 of such options shall vest over
three
years, of which amounts, 1/3 shall vest and be exercisable upon the first
anniversary of the issuance of the options and the remainder shall vest and
be
exercisable on a quarterly basis; (ii) 1/3 of such options shall vest and be
exercisable upon our achieving a total market capitalization on a fully diluted
basis of more than US $350 million; and (iii) 1/3 of such options shall vest
upon our achieving a total market capitalization on a fully diluted basis of
more than US $550 million. The options can be exercised for a period of ten
years. The grant of such options is conditional upon approval of the
shareholders at a duly convened shareholder meeting expected to take place
later
this year.
The
Selling Shareholders received ADRs representing our ordinary shares as the
result of a private placement of our ordinary shares on March 22, 2006. Selling
Shareholders, including any non-sale transferees, pledges or donees or their
successors, may from time to time offer and sell any or all of the ADRs
representing ordinary shares pursuant to this prospectus or any prospectus
supplement.
The
Selling Shareholders may offer all, some or none of the ADRs. Because the
Selling Shareholders may offer all or some portion of the ADRs, no estimate
can
be given as to the amount of ADRs that will be held by the Selling Shareholders
upon termination of any sales.
|
Name
and Address of Selling Shareholder
|
Number
of ADRs representing ordinary shares obtained as the result of the
private
placement and registered hereby (includes ADRs receivable upon the
exercise of Warrants)
|
Number
of ADRs receivable upon the exercise of Warrants
|
Number
of ADRs representing ordinary shares obtained as the result of the
private
placement and registered hereby beneficially owned as of the date
hereof
(1)
|
|||||||
|
Catalytix,
LDC
c/o
CIBC Bank and Trust Company (Cayman) Limited
CIBC
Financial Centre
11
Dr. Roy’s Drive
P.O.
Box 694 GT
Grand
Cayman, Cayman Islands, B.W.I.
|
18,750
|
6,250
|
0
|
|||||||
|
Catalytix
LDC Life Science Hedge AC
c/o
CIBC Bank and Trust Company (Cayman) Limited
CIBC
Financial Centre
11
Dr. Roy’s Drive
P.O.
Box 694 GT
Grand
Cayman, Cayman Islands, B.W.I.
|
18,750
|
6,250
|
0
|
|||||||
|
Formula
Investment House, Ltd.
Trident
Chambers, P.O. Box 146
Road
Town, Tortola
British
Virgin Islands
|
75,000
|
25,000
|
0
|
|||||||
|
GLG
North American Opportunity Fund
Walker
House
P.O.
Box 908GT
George
Town, Grand Cayman
Cayman
Islands
|
249,999
|
83,333
|
0
|
|||||||
|
North
Sound Legacy Institutional Fund LLC
c/o
North Sound Capital LLC
20
Horseneck Lane
Greenwich,
CT 06830
|
210,000
|
70,000
|
0
|
|||||||
|
Name
and Address of Selling Shareholder
|
Number
of ADRs representing ordinary shares obtained as the result of
the private
placement and registered hereby (includes ADRs receivable upon
the
exercise of Warrants)
|
Number
of ADRs receivable upon the exercise of Warrants
|
Number
of ADRs representing ordinary shares obtained as the result of
the private
placement and registered hereby beneficially owned as of the date
hereof
(1)
|
|||||||
|
North
Sound Legacy International Ltd.
c/o
North Sound Capital LLC
20
Horseneck Lane
Greenwich,
CT 06830
|
540,000
|
180,000
|
0
|
|||||||
|
Merlin
Biomed, LP
230
Park Avenue, Suite 928
New
York, NY 10169
|
195,000
|
65,000
|
0
|
|||||||
|
Merlin
Biomed Round Table Fund, LP
230
Park Avenue, Suite 928
New
York, NY 10169
|
11,550
|
3,850
|
0
|
|||||||
|
Merlin
Biomed II, LP
230
Park Avenue, Suite 928
New
York, NY 10169
|
57,949.5
|
19,316.5
|
0
|
|||||||
|
Merlin
Biomed International, Ltd.
230
Park Avenue, Suite 928
New
York, NY 10169
|
235,500
|
78,500
|
0
|
|||||||
|
Capital
Ventures International
c/o
Heights Capital Management, Inc.
101
California Street, Suite 3250
San
Francisco, CA 94111
|
124,999.5
|
41,666.5
|
0
|
|||||||
|
RAQ,
LLC
787
Seventh Ave., 48th
Floor
New
York, NY 10019
|
62,500.5
|
20,833.5
|
0
|
|||||||
|
Valesco
Healthcare Partners I LP
787
Seventh Ave., 48th
Floor
New
York, NY 10019
|
21,000
|
7,000
|
0
|
|||||||
|
Valesco
Healthcare Partners II LP
787
Seventh Ave., 48th
Floor
New
York, NY 10019
|
43,999.5
|
14,666.5
|
0
|
|||||||
|
Valesco
Healthcare Overseas Fund, Ltd.
787
Seventh Ave., 48th
Floor
New
York, NY 10019
|
34,999.5
|
11,666.5
|
0
|
|||||||
|
Fore
Convertible Master Fund, Ltd.
c/o
Fore Research & Management, L.P.
280
Park Avenue, 43rd
Floor
New
York, NY 10017
|
323,100
|
107,700
|
0
|
|||||||
|
Fore
Multi Strategy Master Fund, Ltd.
c/o
Fore Research & Management, L.P.
280
Park Avenue, 43rd
Floor
New
York, NY 10017
|
201,450
|
67,150
|
0
|
|||||||
|
Fore
Erisa Fund, Ltd.
c/o
Fore Research & Management, L.P.
280
Park Avenue, 43rd
Floor
New
York, NY 10017
|
39,450
|
13,150
|
0
|
|
Name
and Address of Selling Shareholder
|
Number
of ADRs representing ordinary shares obtained as the result of
the private
placement and registered hereby (includes ADRs receivable upon
the
exercise of Warrants)
|
Number
of ADRs receivable upon the exercise of Warrants
|
Number
of ADRs representing ordinary shares obtained as the result of
the private
placement and registered hereby beneficially owned as of the date
hereof
(1)
|
|||||||
|
Man
Mac 1, Ltd.
c/o
Fore Research & Management, L.P.
280
Park Avenue, 43rd
Floor
New
York, NY 10017
|
186,000
|
62,000
|
0
|
|||||||
|
Narragensett
I, LP
540
Madison Avenue, 38th
Floor
New
York, NY 10022
|
360,000
|
120,000
|
0
|
|||||||
|
Narragensett
Offshore, Ltd.
540
Madison Avenue, 38th
Floor
New
York, NY 10022
|
390,000
|
130,000
|
0
|
|||||||
|
Highbridge
International LLC
c/o
Highbridge Capital Management, LLC
9
W. 57th
Street, 27th
Floor
New
York, NY 10019
|
750,000
|
250,000
|
0
|
|||||||
|
Portside
Growth and Opportunity Fund
c/o
Ramius Capital Group, LLC
666
Third Avenue, 26th
Floor
New
York, NY 10017
|
249,999
|
83,333
|
0
|
|||||||
|
Senvest
Master Fund LP
110
East 55th
Street, Suite 1600
New
York, NY 10022
|
156,499.5
|
52,166.5
|
0
|
|||||||
|
Senvest
Israel Partners LP
110
East 55th
Street, Suite 1600
New
York, NY 10022
|
156,000
|
52,000
|
0
|
|||||||
|
Sonostar
Capital Partners LLC
191
King Street
Chappaqua,
NY 10514
|
124,999.5
|
41,666.5
|
0
|
|||||||
|
Kenneth
Hoberman
28
Avenue at Port Imperial #327
West
New York, NJ 07657
|
63,501
|
21,167
|
0
|
|||||||
|
Nortrust
Nominees Ltd.
c/o
Invesco Asset Management
30
Finsbury Square
London,
England EC2A 1AG
|
1,206
|
402
|
0
|
|||||||
|
Chase
Nominees Ltd.
c/o
Invesco Asset Management
30
Finsbury Square
London,
England EC2A 1AG
|
43,812
|
14,604
|
0
|
|||||||
|
Vioacos
Nominees Limited
c/o
Invesco Asset Management
30
Finsbury Square
London,
England EC2A 1AG
|
7,797
|
2,599
|
0
|
|
Name
and Address of Selling Shareholder
|
Number
of ADRs representing ordinary shares obtained as the result of
the private
placement and registered hereby (includes ADRs receivable upon
the
exercise of Warrants)
|
Number
of ADRs receivable upon the exercise of Warrants
|
Number
of ADRs representing ordinary shares obtained as the result of
the private
placement and registered hereby beneficially owned as of the date
hereof
(1)
|
|||||||
|
Vioacos
Nominees Limited
c/o
Invesco Asset Management
30
Finsbury Square
London,
England EC2A 1AG
|
142,185
|
47,395
|
0
|
|||||||
|
James
Oliviero III
220
Riverside Boulevard, #6A
New
York, NY 10069
|
16,509
|
5,503
|
0
|
|||||||
|
Diamondback
Master Fund, Ltd.
One
Landmark Square - 15th
Floor
Stamford,
CT 06901
|
249,999
|
83,333
|
0
|
|||||||
|
Cimarron
Biomedical Equity Master Fund L.P.
2626
Cole Avenue, Suite 400
Dallas,
TX 75204
|
75,000
|
25,000
|
0
|
|||||||
|
Rock
Securities Limited
20
Balderton Street - 4th
Floor
London,
England WIK 6TL
|
124,999.5
|
41,666.5
|
0
|
|||||||
|
Iroquois
Master Fund Ltd.
641
Lexington Avenue, 26th
Floor
New
York, NY 10022
|
187,500
|
62,500
|
0
|
|||||||
|
Bank
Julius Baer & Co. Ltd.
Bahnhofstrasse
36
P.O.
Box
CH-8010
Zurish
|
999,999
|
333,333
|
0
|
|||||||
|
Apex
Investments Ltd.
2
Koyfman Street
Tel-Aviv,
Israel 68012
|
49,999.5
|
16,666.5
|
0
|
|||||||
|
Apex
Provident Funds
2
Koyfman Street
Tel-Aviv,
Israel 68012
|
49,999.5
|
16,666.5
|
0
|
|||||||
|
Yourdent
Ltd.
Sharet
1/26
Natanya,
Israel
|
49,999.5
|
16,666.5
|
0
|
|||||||
|
Aviv
Raiz
17
Haarbaa Street
Tel
Aviv, Israel
|
99,999
|
33,333
|
0
|
|||||||
|
Total
|
7,000,000.5
|
2,333,333.5
|
0
|
___________________________________
(1) Assumes
sale of all of the ADRs representing ordinary shares obtained as a result of
the
private placement, registered and offered hereby.
The
Selling Shareholders and any of their pledgees, assignees and
successors-in-interest may, from time to time, sell any or all of their ADRs
on
any stock exchange, market or trading facility on which the ADRs are traded
or
in private transactions. These sales may be at fixed or negotiated prices.
The
Selling Shareholders may use any one or more of the following methods when
selling ADRs:
|
·
|
ordinary
brokerage transactions and transactions in which the broker-dealer
solicits purchasers;
|
|
·
|
block
trades in which the broker-dealer will
attempt
to sell the ADRs as agent but may position and resell a portion of
the
block as principal to facilitate the transaction;
|
|
·
|
purchases
by a broker-dealer as principal and resale by the broker-dealer for
its
account;
|
|
·
|
an
exchange distribution in accordance with the rules of the applicable
exchange;
|
|
·
|
privately
negotiated transactions;
|
|
·
|
settlement
of short sales created
after the date of the private placement;
|
|
·
|
broker-dealers
may agree with the Selling Shareholders to sell a specified number
of such
ADRs at a stipulated price per ADR;
|
|
·
|
a
combination of any such methods of sale; and
|
|
·
|
any
other method permitted pursuant to applicable
law.
|
The
Selling Shareholders may also sell shares under Rule 144 under the Securities
Act, if available, rather than under this prospectus. Broker-dealers engaged
by
the Selling Shareholders may arrange for other brokers dealers to participate
in
sales. Broker-dealers may receive commissions or discounts from the Selling
Shareholders (or, if any broker-dealer acts as agent for the purchaser of ADRs,
from the purchaser) in amounts to be negotiated. The Selling Shareholders do
not
expect these commissions and discounts to exceed what is customary in the types
of transactions involved.
The
Selling Shareholders may from time to time pledge or grant a security interest
in some or all of the ADRs owned by them and, if they default in the performance
of their secured obligations, the pledgees or secured parties may offer and
sell
the ADRS from time to time under this prospectus, or under an amendment to
this
prospectus under Rule 424(b)(3) or other applicable provision of the Securities
Act of 1933 amending the list of Selling Shareholders to include the pledgee,
transferee or other successors in interest as Selling Shareholders under this
prospectus.
The
Selling Shareholders also may transfer the ADRs in other circumstances, in
which
case the transferees, pledgees or other successors in interest will be the
selling beneficial owners for purposes of this prospectus.
The
Selling Shareholders and any broker-dealers or agents that are involved in
selling the ADRs may be deemed to be “underwriters” within the meaning of the
Securities Act in connection with such sales. In such event, any commissions
received by such broker-dealers or agents and any profit on the resale of the
ADRs purchased by them may be deemed to be underwriting commissions or discounts
under the Securities Act. The Selling Shareholders have informed us that none
of
them have any agreement or understanding, directly or indirectly, with any
person to distribute the ADRs.
We
are
required to pay all fees and expenses that we incur incident to the registration
of the ADRs. We have agreed to indemnify the Selling Shareholders against
certain losses, claims, damages and liabilities, including liabilities under
the
Securities Act.
The
table
below itemizes the expenses payable by us in connection with the registration
and issuance of the securities being registered by this prospectus. All amounts
except the Securities and Exchange Commission registration fee are
estimated.
|
Placement
Agents
|
$
|
2,510,000
|
||
|
Securities
and Exchange Commission Registration Fee
|
$
|
5,540
|
||
|
Legal
Fees and Expenses
|
$
|
704,460
|
|
|
|
Accountants'
Fees and Expenses
|
$
|
305,000
|
||
|
Printing
and Duplicating Expenses
|
$
|
30,000
|
||
|
Miscellaneous
Expenses
|
$
|
45,000
|
||
|
Total
|
$
|
3,600,000
|
The
following table sets forth certain information regarding beneficial ownership
of
our ordinary shares as of March 31, 2006, by each person who is known by us
to
own beneficially more than 5% of our outstanding ordinary shares. The voting
rights of our major shareholders do not differ from the voting rights of other
holders of our ordinary shares.
|
Beneficial
owner
|
Number
of ordinary shares beneficially owned (1)
|
Percent
of
ownership
(1)
|
|||||
|
Bank
Julius Baer
|
15,369,644
|
8.87
|
%
|
||||
|
Perpetual
Income & Growth Investment Trust Inc.
|
13,732,146
|
7.93
|
%
|
||||
| (1) |
Does
not include ADRs representing ordinary shares obtained as a result
of the
private placement that we completed on March 22,
2006.
|
As
of
March 31, 2006, there were a total of 484 holders of record of our ordinary
shares, of which 29 were registered with addresses in the United States. Such
United States holders were, as of such date, the holders of record of
approximately 6% of the outstanding ordinary shares.
Share
Capital
As
of
March 31, 2006, we had 300,000,000 ordinary shares, par value NIS 0.02,
authorized and 173,272,364
ordinary
shares issued and outstanding. All of the outstanding shares are issued and
fully paid, and exclude the recent private placement that closed in March
2006.
As
of
March 31, 2006, an additional 31,684,192 ordinary shares are issuable upon
the
exercise of outstanding options and warrants to purchase our ordinary shares.
The exercise price of the options and warrants outstanding is between $0.106
and
$2.110 per share. In addition see "Management - Directors, Senior Management
and
Employees - Share Ownership - Share Option Plans" above, for a more detailed
discussion on options that were granted to employees, directors and
consultants.
As
of
December 31, 2002, we had 300,000,000 ordinary shares, par value NIS 0.02,
authorized and 111,165,364 ordinary shares issued and outstanding. Since such
date and through December 31, 2005, we have issued an aggregate of 4,690,925
ordinary shares upon the exercise of options. In addition, in August 2004,
we
issued 56,009,732 ordinary shares pursuant to a placing and open offer for
new
ordinary shares on the London Stock Exchange and in September 2005, we issued
1,314,420 ordinary shares pursuant to a license agreement and an asset purchase
agreement with VivoQuest Inc.
Memorandum
and Articles of Association
Objects
and Purposes of the Company
Pursuant
to Part B, Section 3 of our Articles of Association, we may undertake any lawful
activity.
Powers
and Obligations of the Directors
Pursuant
to the Israeli Companies Law and our Articles of Association, a director is
not
permitted to vote on a proposal, arrangement or contract in which he or she
has
a personal interest. Also, the directors may not vote compensation to themselves
or any members of their body, as that term is defined under Israeli law, without
the approval of our audit committee and our shareholders at a general meeting.
The requirements for approval of certain transactions are set forth below in
“Share Capital - Additional Information-Memorandum and Articles of
Association-Approval of Certain Transactions.” The power of our directors to
enter into borrowing arrangements on our behalf is limited to the same extent
as
any other transaction by us.
The
Israeli Companies Law codifies the fiduciary duties that office holders,
including directors and executive officers, owe to a company. An office holder’s
fiduciary duties consist of a duty of care and a duty of loyalty. The duty
of
care generally requires an office holder to act with the same level of care
as a
reasonable office holder in the same position would employ under the same
circumstances. The duty of loyalty includes avoiding any conflict of interest
between the office holder’s position in the company and such person’s personal
affairs, avoiding any competition with the company, avoiding exploiting any
corporate opportunity of the company in order to receive personal advantage
for
such person or others, and revealing to the company any information or documents
relating to the company’s affairs which the office holder has received due to
his or her position as an office holder.
Indemnification
of Directors and Officers; Limitations on Liability
Israeli
law permits a company to insure an office holder in respect of liabilities
incurred by him or her as a result of an act or omission in the capacity of
an
office holder for:
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a
breach of the office holder’s duty of care to the company or to another
person;
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a
breach of the office holder’s fiduciary duty to the company, provided that
he or she acted in good faith and had reasonable cause to believe
that the
act would not prejudice the company; and
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a
financial liability imposed upon the office holder in favor of another
person.
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Moreover,
a company can indemnify an office holder for any of the following obligations
or
expenses incurred in connection with the acts or omissions of such person in
his
or her capacity as an office holder:
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monetary
liability imposed upon him or her in favor of a third party by a
judgment,
including a settlement or an arbitral award confirmed by the court;
and
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reasonable
litigation expenses, including attorneys’ fees, actually incurred by the
office holder or imposed upon him or her by a court, in a proceeding
brought against him or her by or on behalf of the company or by a
third
party, or in a criminal action in which he or she was acquitted,
or in a
criminal action which does not require criminal intent in which he
or she
was convicted; furthermore, a company can, with a limited exception,
exculpate an office holder in advance, in whole or in part, from
liability
for damages sustained by a breach of duty of care to the
company.
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Our
Articles of Association allow for insurance, exculpation and indemnification
of
office holders to the fullest extent permitted by law. We have entered into
indemnification, insurance and exculpation agreements with our directors and
executive officers, following shareholder approval of these agreements. We
have
directors’ and officers’ liability insurance covering our officers and directors
for a claim imposed upon
them
as a result of an action carried out while serving as an officer or director,
for (a) the breach of duty of care towards us or towards another person, (b)
the
breach of fiduciary duty towards us, provided that the officer or director
acted
in good faith and had reasonable grounds to assume that the action would not
harm our interests, and (c) a monetary liability imposed upon him in favor
of a
third party.
Approval
of Certain Transactions
The
Israeli Companies Law codifies the fiduciary duties that office holders,
including directors and executive officers, owe to a company. An office holder,
as defined in the Israeli Companies Law, is a director, general manager, chief
business manager, deputy general manager, vice general manager, executive vice
president, vice president, other manager directly subordinate to the managing
director or any other person assuming the responsibilities of any of the
foregoing positions without regard to such person's title. An office holder's
fiduciary duties consist of a duty of care and a duty of loyalty. The duty
of
loyalty includes avoiding any conflict of interest between the office holder's
position in the company and his personal affairs, avoiding any competition
with
the company, avoiding exploiting any business opportunity of the company in
order to receive personal advantage for himself or others, and revealing to
the
company any information or documents relating to the company's affairs which
the
office holder has received due to his position as an office holder. Each person
listed in the table under “Directors and Senior Management,” which is displayed
under “Management - Directors, Senior Management and Employees-Directors and
Senior Management,” is an office holder of XTLbio. Under the Israeli Companies
Law, all arrangements as to compensation of office holders who are not directors
require approval of the board of directors, or a committee thereof. Arrangements
regarding the compensation of directors also require audit committee and
shareholders approval, with the exception of compensation to external directors
in the amounts specified in the regulations discussed in “Management - Directors
and Senior Management-Compensation.”
The
Israeli Companies Law requires that an office holder promptly discloses any
personal interest that he or she may have, and all related material information
known to him or her, in connection with any existing or proposed transaction
by
the company. The disclosure must be made to our board of directors or
shareholders without delay and prior to the meeting at which the transaction
is
to be discussed. In addition, if the transaction is an extraordinary
transaction, as defined under the Israeli Companies Law, the office holder
must
also disclose any personal interest held by the office holder's spouse,
siblings, parents, grandparents, descendants, spouse's descendants and the
spouses of any of the foregoing, or by any corporation in which the office
holder is a 5% or greater shareholder, or holder of 5% or more of the voting
power, director or general manager or in which he or she has the right to
appoint at least one director or the general manager. An extraordinary
transaction is defined as a transaction not in the ordinary course of business,
not on market terms, or that is likely to have a material impact on the
company's profitability, assets or liabilities.
In
the
case of a transaction which is not an extraordinary transaction (other than
transactions relating to a director’s conditions of service), after the office
holder complies with the above disclosure requirement, only board approval
is
required unless the Articles of Association of the company provides otherwise.
The transaction must not be adverse to the company's interest. If the
transaction is an extraordinary transaction, then, in addition to any approval
required by the Articles of Association, the transaction must also be approved
by the audit committee and by the board of directors, and under specified
circumstances, by a meeting of the shareholders. An office holder who has a
personal interest in a matter that is considered at a meeting of the board
of
directors or the audit committee may not be present at this meeting or vote
on
this matter.
The
Israeli Companies Law applies the same disclosure requirements to a controlling
shareholder of a public company, which is defined as a shareholder who has
the
ability to direct the activities of a company, other than in circumstances
where
this power derives solely from the shareholder’s position on the Board or any
other position with the company, and includes a shareholder that holds 25%
or
more of the voting rights if no other shareholder owns more than 50% of the
voting rights in the company. Extraordinary transactions with a controlling
shareholder or in which a controlling shareholder has a personal interest,
and
the terms of compensation of a controlling shareholder who is an office holder,
require the approval of the audit committee, the board of directors and the
shareholders of the company. The shareholders’ approval must either include at
least one-third of the disinterested shareholders who are present, in person
or
by proxy, at the meeting, or, alternatively, the total shareholdings of the
disinterested shareholders who vote against the transaction must not represent
more than one percent of the voting rights in the company.
In
addition, a private placement of securities that will increase the relative
holdings of a shareholder that holds 5% or more of the company’s outstanding
share capital, assuming the exercise by such person of all of the convertible
securities into shares held by that person, or that will cause any person to
become a holder of more than 5% of the company’s outstanding share capital,
requires approval by the board of directors and the shareholders of the company.
However, subject to certain exceptions under regulations adopted under the
Israeli Companies Law, shareholder approval will not be required if the
aggregate number of shares issued pursuant to such private placement, assuming
the exercise of all of the convertible securities into shares being sold in
such
a private placement, comprises less than 20% of the voting rights in a company
prior to the consummation of the private placement.
Under
the
Israeli Companies Law, a shareholder has a duty to act in good faith towards
the
company and other shareholders and refrain from abusing his power in the
company, including, among other things, voting in the general meeting of
shareholders on the following matters:
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any
amendment to the Articles of Association;
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an
increase of the company's authorized share capital;
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a
merger; and
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approval
of interested party transactions that require shareholders
approval.
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In
addition, any controlling shareholder, any shareholder who knows it can
determine the outcome of a shareholders vote and any shareholder who, under
a
company’s Articles of Association, can appoint or prevent the appointment of an
office holder, is under a duty to act with fairness towards the company. The
Israeli Companies Law does not describe the substance of this duty. The Israeli
Companies Law requires that specified types of transactions, actions and
arrangements be approved as provided for in a company’s articles of association
and in some circumstances by the audit committee, by the board of directors
and
by the shareholders. In general, the vote required by the audit committee and
the board of directors for approval of these matters, in each case, is a
majority of the disinterested directors participating in a duly convened
meeting.
Rights
Attached to Ordinary Shares
Our
authorized share capital consists of 300,000,000 ordinary shares, par value
NIS
0.02 per share.
Holders
of ordinary shares have one vote per share, and are entitled to participate
equally in the payment of dividends and share distributions and, in the event
of
our liquidation, in the distribution of assets after satisfaction of liabilities
to creditors. No preferred shares are currently authorized. All outstanding
ordinary shares are validly issued and fully paid.
Transfer
of Shares
Fully
paid ordinary shares are issued in registered form and may be freely transferred
under our Articles of Association unless the transfer is restricted or
prohibited by another instrument or applicable securities laws.
Dividend
and Liquidation Rights
We
may
declare a dividend to be paid to the holders of ordinary shares according to
their rights and interests in our profits. In the event of our liquidation,
after satisfaction of liabilities to creditors, our assets will be distributed
to the holders of ordinary shares in proportion to the nominal value of their
holdings.
This
right may be affected by the grant of preferential dividend or distribution
rights, to the holders of a class of shares with preferential rights that may
be
authorized in the future. Under the Israeli Companies Law, the declaration
of a
dividend does not require the approval of the shareholders of the company,
unless the company's Articles of Association require otherwise. Our Articles
of
Association provide that the board of directors may declare and distribute
dividends without the approval of the shareholders.
Annual
and Extraordinary General Meetings
We
must
hold our annual general meeting of shareholders each year no later than 15
months from the last annual meeting, at a time and place determined by the
board
of directors, upon at least 21 days’ prior notice to our shareholders to which
we need to add additional three days for notices sent outside of Israel. A
special meeting may be convened by request of two directors, 25% of the
directors then in office, one or more shareholders holding at least 5% of our
issued share capital and at least 1% of our issued voting rights, or one or
more
shareholders holding at least 5% of our issued voting rights. Notice of a
general meeting must set forth the date, time and place of the meeting. Such
notice must be given at least 21 days but not more than 45 days prior to the
general meeting. The quorum required for a meeting of shareholders consists
of
at least two shareholders present in person or by proxy who hold or represent
between them at least one-third of the voting rights in the company. A meeting
adjourned for lack of a quorum generally is adjourned to the same day in the
following week at the same time and place (with no need for any notice to the
shareholders) or until such other later time if such time is specified in the
original notice convening the general meeting, or if we serve notice to the
shareholders no less than seven days before the date fixed for the adjourned
meeting. If at an adjourned meeting there is no quorum present half an hour
after the time set for the meeting, any number participating in the meeting
shall represent a quorum and shall be entitled to discuss the matters set down
on the agenda for the original meeting. All
shareholders who are registered in our registrar on the record date, or who
will
provide us with proof of ownership on that date as applicable to the relevant
registered shareholder, are entitled to participate in a general meeting and
may
vote as described in “Voting Rights” and “Voting by Proxy and in Other Manners”
below.
Voting
Rights
Our
ordinary shares do not have cumulative voting rights in the election of
directors. As a result, the holders of ordinary shares that represent more
than
50% of the voting power represented at a shareholders meeting in which a quorum
is present have the power to elect all of our directors, except the external
directors whose election requires a special majority as described under the
section entitled “Board Practices - External and Independent
Directors.”
Holders
of ordinary shares have one vote for each ordinary share held on all matters
submitted to a vote of shareholders. Shareholders may vote in person or by
proxy. These voting rights may be affected by the grant of any special voting
rights to the holders of a class of shares with preferential rights that may
be
authorized in the future.
Under
the
Israeli Companies Law, unless otherwise provided in the Articles of Association
or by applicable law, all resolutions of the shareholders require a simple
majority. Our Articles of Association provide that all decisions may be made
by
a simple majority. See “-Approval of Certain Transactions” above for certain
duties of shareholders towards the company.
Voting
by Proxy and in Other Manners
Our
Articles of Association enable a shareholder to appoint a proxy, who need not
be
a shareholder, to vote at any shareholders meeting. We require that the
appointment of a proxy be in writing signed by the person making the appointment
or by an attorney authorized for this purpose, and if the person making the
appointment is a corporation, by a person or persons authorized to bind the
corporation. In the document appointing a proxy, each shareholder may specify
how the proxy should vote on any matter presented at a shareholders meeting.
The
document appointing the proxy shall be deposited in our offices or at such
other
address as shall be specified in the notice of the meeting not less than 48
hours before the time of the meeting at which the person specified in the
appointment is due to vote.
The
Israeli Companies Law and our Articles of Association do not permit resolutions
of the shareholders to be adopted by way of written consent, for as long as
our
ordinary shares are publicly traded.
Limitations
on the Rights to Own Securities
The
ownership or voting of ordinary shares by non-residents of Israel is not
restricted in any way by our Articles of Association or the laws of the State
of
Israel, except that nationals of countries which are, or have been, in a state
of war with Israel may not be recognized as owners of ordinary
shares.
Anti-Takeover
Provisions under Israeli Law
The
Israeli Companies Law permits merger transactions with the approval of each
party’s board of directors and shareholders. In accordance with the Israeli
Companies Law, a merger may be approved at a shareholders meeting by a majority
of the voting power represented at the meeting, in person or by proxy, and
voting on that resolution. In determining whether the required majority has
approved the merger, shares held by the other party to the merger, any person
holding at least 25% of the outstanding voting shares or means of appointing
the
board of directors of the other party to the merger, or the relatives or
companies controlled by these persons, are excluded from the vote.
Under
the
Israeli Companies Law, a merging company must inform its creditors of the
proposed merger. Any creditor of a party to the merger may seek a court order
blocking the merger, if there is a reasonable concern that the surviving company
will not be able to satisfy all of the obligations of the parties to the merger.
Moreover, a merger may not be completed until at least 30 days have passed
from
the time the merger was approved in a general meeting of each of the merging
companies, and at least 50 days have passed from the time that a merger proposal
was filed with the Israeli Registrar of Companies.
The
Israeli Companies Law provides that an acquisition of shares in a public company
must be made by means of a tender offer if, as a result of such acquisition,
the
purchaser would become shareholder with over 25% of the voting rights in the
company. This rule does not apply if there is already another shareholder of
the
company with 25% or more of the voting rights. Similarly, the Israeli Companies
Law provides that an acquisition of shares in a public company must be made
by
means of a tender offer if, as a result of the acquisition, the purchaser’s
shareholdings would entitle the purchaser to over 45% of the voting rights
in
the company, unless there is a shareholder with 50% or more of the voting rights
in the company. These rules do not apply if the acquisition is made by way
of a
merger. Regulations promulgated under the Israeli Companies Law provide that
these tender offer requirements do not apply to companies whose shares are
listed for trading external of Israel if, according to the law in the country
in
which the shares are traded, including the rules and regulations of the stock
exchange or which the shares are traded, either:
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there
is a limitation on acquisition of any level of control of the company;
or
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the
acquisition of any level of control requires the purchaser to do
so by
means of a tender offer to the
public.
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The
Israeli Companies Law provides specific rules and procedures for the acquisition
of shares held by minority shareholders, if the majority shareholder holds
more
than 90% of the outstanding shares. Israeli tax law treats specified
acquisitions, including a stock-for-stock swap between an Israeli company and
a
foreign company, less favorably than does U.S. tax law. These laws may have
the
effect of delaying or deterring a change in control of us, thereby limiting
the
opportunity for shareholders to receive a premium for their shares and possibly
affecting the price that some investors are willing to pay for our
securities.
Rights
of Shareholders
Under
the
Israeli Companies Law, our shareholders have the right to inspect certain
documents and registers including the minutes of general meetings, the register
of shareholders and the register of substantial shareholders, any document
held
by us that relates to an act or transaction requiring the consent of the general
meeting as stated above under “-Approval of Certain Transactions,” our Articles
of Association and our financial statements, any other document which we are
required to file under the Israeli Companies Law or under any law with the
Registrar of Companies or the Israeli Securities Authority, and is available
for
public inspection at the Registrar of Companies or the Securities Authority,
as
the case may be.
If
the
document required for inspection by one of our shareholders relates to an act
or
transaction requiring the consent of the general meeting as stated above, we
may
refuse the request of the shareholder if in our opinion the request was not
made
in good faith, the documents requested contain a commercial secret or a patent,
or disclosure of the documents could prejudice our good in some other
way.
The
Israeli Companies Law provides that with the approval of the court any of our
shareholders or directors may file a derivative action on our behalf if the
court finds the action is a priori, to our benefit, and the person demanding
the
action is acting in good faith. The demand to take action can be filed with
the
court only after it is serviced to us, and we decline or omit to act in
accordance to this demand.
Enforceability
of Civil Liabilities
We
are
incorporated in Israel and some of our directors and officers and the Israeli
experts named in this prospectus reside outside the United States. Service
of
process upon them may be difficult to effect within the United States.
Furthermore, because substantially all of our assets, and those of our
non-United States directors and officers and the Israeli experts named herein,
are located outside the United States, any judgment obtained in the United
States against us or any of these persons may not be collectible within the
United States.
We
have
been informed by our legal counsel in Israel, Kantor & Co, that there is
doubt as to the enforceability of civil liabilities under the Securities Act
or
the Exchange Act, pursuant to original actions instituted in Israel. However,
subject to particular time limitations, executory judgments of a United States
court for monetary damages in civil matters may be enforced by an Israeli court,
provided that:
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the
judgment was obtained after due process before a court of competent
jurisdiction, that recognizes and enforces similar judgments of Israeli
courts, and the court had authority according to the rules of private
international law currently prevailing in Israel;
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adequate
service of process was effected and the defendant had a reasonable
opportunity to be heard;
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the
judgment is not contrary to the law, public policy, security or
sovereignty of the State of Israel and its enforcement is not contrary
to
the laws governing enforcement of judgments;
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the
judgment was not obtained by fraud and does not conflict with any
other
valid judgment in the same matter between the same
parties;
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the
judgment is no longer appealable; and
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an
action between the same parties in the same matter is not pending
in any
Israeli court at the time the lawsuit is instituted in the foreign
court.
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We
have
irrevocably appointed XTL Biopharmaceuticals, Inc., our U.S. subsidiary, as
our
agent to receive service of process in any action against us in any United
States federal court or the courts of the State of New York arising out of
any
purchase or sale of ADRs representing ordinary shares offered by the Selling
Shareholders.
Foreign
judgments enforced by Israeli courts generally will be payable in Israeli
currency. The usual practice in an action before an Israeli court to recover
an
amount in a non-Israeli currency is for the Israeli court to render judgment
for
the equivalent amount in Israeli currency at the rate of exchange in force
on
the date of the judgment. Under existing Israeli law, a foreign judgment payable
in foreign currency may be paid in Israeli currency at the rate of exchange
for
the foreign currency published on the day before date of payment. Current
Israeli exchange control regulations also permit a judgment debtor to make
payment in foreign currency. Pending collection, the amount of the judgment
of
an Israeli court stated in Israeli currency ordinarily may be linked to Israel’s
consumer price index plus interest at the annual statutory rate set by Israeli
regulations prevailing at that time. Judgment creditors must bear the risk
of
unfavorable exchange rates.
Exchange
Controls
Under
Israeli Law, Israeli non-residents who purchase ordinary shares with certain
non-Israeli currencies (including dollars) may freely repatriate in such
non-Israeli currencies all amounts received in Israeli currency in respect
of
the ordinary shares, whether as a dividend, as a liquidating distribution,
or as
proceeds from any sale in Israel of the ordinary shares, provided in each case
that any applicable Israeli income tax is paid or withheld on such amounts.
The
conversion into the non-Israeli currency must be made at the rate of exchange
prevailing at the time of conversion.
Legal
Proceedings
Neither
we nor our subsidiary is a party to, and our property is not the subject of,
any
material pending legal proceedings.
American
Depository Shares
On
the
effective date of the registration statement of which this prospectus is a
part,
we issued and deposited the ordinary shares registered hereby with Bank Hapoalim
B.M., The Bank of New York’s custodian in Tel Aviv, Israel. The Bank of New York
in turn issued to the Selling Shareholders American Depositary Receipts, or
ADRs, representing American Depositary Shares, or ADSs. One ADR represents
an
ownership interest in ten of our ordinary shares. Each ADR also represents
securities, cash or other property deposited with The Bank of New York but
not
distributed to ADR holders. The Bank of New York's Corporate Trust Office is
located at 101 Barclay Street, New York, NY 10286, U.S.A. Their principal
executive office is located at One Wall Street, New York, NY 10286,
U.S.A.
You
may
hold ADRs either directly or indirectly through your broker or other financial
institution. If you hold ADRs directly, you are an ADR holder. This description
assumes you hold your ADRs directly. If you hold the ADRs indirectly, you must
rely on the procedures of your broker or other financial institution to assert
the rights of ADR holders described in this section. You should consult with
your broker or financial institution to find out what those procedures are.
Because
The Bank of New York will actually hold the ordinary shares, you must rely
on it
to exercise the rights of a shareholder. The obligations of The Bank of New
York
are set out in a deposit agreement among us, The Bank of New York and you,
as an
ADR holder. The agreement and the ADRs are generally governed by New York
law.
The
following is a summary of the agreement. Because it is a summary, it does not
contain all the information that may be important to you. For more complete
information, you should read the entire agreement and the ADR. Directions on
how
to obtain copies of these are provided in the section entitled "Where You Can
Find More Information."
Share
Dividends and Other Distributions
The
Bank
of New York has agreed to pay to you the cash dividends or other distributions
it or the custodian receives on shares or other deposited securities after
deducting its fees and expenses. You will receive these distributions in
proportion to the number of shares your ADRs represent.
Cash.
The Bank
of New York will convert any cash dividend or other cash distribution we pay
on
the shares into U.S. dollars, if it can do so on a reasonable basis and can
transfer the U.S. dollars to the U.S. If that is not possible or if any approval
from any government or agency thereof is needed and cannot be obtained, the
agreement allows The Bank of New York to distribute the foreign currency only
to
those ADR holders to whom it is possible to do so. It will hold the foreign
currency it cannot convert for the account of the ADR holders who have not
been
paid. It will not invest the foreign currency and it will not be liable for
the
interest.
Before
making a distribution, any withholding taxes that must be paid under U.S. law
will be deducted. See “Taxation—United States Federal Income Tax
Considerations—Taxation of Dividends Paid On Ordinary Shares.” The Bank of New
York will distribute only whole U.S. dollars and cents and will round fractional
cents to the nearest whole cent. If the exchange rates fluctuate during a time
when The Bank of New York cannot convert the foreign currency, you may lose
some
or all of the value of the distribution.
Shares.
The
Bank
of New York may distribute new ADRs representing any shares we may distribute
as
a dividend or free distribution, if we furnish it promptly with satisfactory
evidence that it is legal to do so. The Bank of New York will only distribute
whole ADRs. It will sell shares which would require it to use a fractional
ADR
and distribute the net proceeds in the same way as it does with cash. If The
Bank of New York does not distribute additional ADRs, each ADR will also
represent the new shares.
Rights
to receive additional shares.
If we
offer holders of our ordinary shares any rights to subscribe for additional
shares or any other rights, The Bank of New York may make these rights available
to you. We must first instruct The Bank of New York to do so and furnish it
with
satisfactory evidence that it is legal to do so. If we do not furnish this
evidence and/or give these instructions, and The Bank of New York decides it
is
practical to sell the rights, The Bank of New York will sell the rights and
distribute the proceeds, in the same way as it does with cash. The Bank of
New
York may allow rights that are not distributed or sold to lapse. In that case,
you will receive no value for them. If The Bank of New York makes rights
available to you, upon instruction from you, it will exercise the rights and
purchase the shares on your behalf. The Bank of New York will then deposit
the
shares and issue ADRs to you. It will only exercise rights if you pay it the
exercise price and any other charges the rights require you to pay.
U.S.
securities laws may restrict the sale, deposit, cancellation and transfer of
the
ADRs issued after exercise of rights. For example, you may not be able to trade
the ADRs freely in the U.S. In this case, The Bank of New York may issue the
ADRs under a separate restricted deposit agreement which will contain the same
provisions as the agreement, except for the changes needed to put the
restrictions in place.
Other
Distributions.
The
Bank of New York will send to you anything else we distribute on deposited
securities by any means it thinks is legal, fair and practical. If it cannot
make the distribution in that way, The Bank of New York has a choice. It may
decide to sell what we distributed and distribute the net proceeds in the same
way as it does with cash or it may decide to hold what we distributed, in which
case the ADRs will also represent the newly distributed property.
The
Bank
of New York is not responsible if it decides that it is unlawful or impractical
to make a distribution available to any ADR holders. We have no obligation
to
register ADRs, shares, rights or other securities under the Securities Act.
We
also have no obligation to take any other action to permit the distribution
of
ADRs, shares, rights or anything else to ADR holders. This means that you may
not receive the distribution we make on our shares or any value for them if
it
is illegal or impractical for us to make them available to you.
Deposit,
Withdrawal and Cancellation
The
Bank
of New York will issue ADRs if you or your broker deposit shares or evidence
of
rights to receive shares with the custodian upon payment of its fees and
expenses and of any taxes or charges, such as stamp taxes or stock transfer
taxes or fees. The Bank of New York will register the appropriate number of
ADRs
in the names you request and will deliver the ADRs at its office to the persons
you request.
You
may
turn in your ADRs at The Bank of New York's office. Upon payment of its fees
and
expenses and of any taxes or charges, such as stamp taxes or stock transfer
taxes or fees, The Bank of New York will deliver (1) the underlying shares
to an
account designated by you and (2) any other deposited securities underlying
the
ADR at the office of the custodian; or, at your request, risk and expense,
The
Bank of New York will deliver the deposited securities at its
office.
Voting
Rights
You
may
instruct The Bank of New York to vote the shares underlying your ADRs but only
if we ask The Bank of New York to ask for your instructions. Otherwise, you
won't be able to exercise your right to vote unless you withdraw the shares.
However, you may not know about the meeting enough in advance to withdraw the
shares.
If
we ask
for your instructions, The Bank of New York will notify you of the upcoming
vote
and arrange to deliver our voting materials to you. The materials will (1)
describe the matters to be voted on and (2) explain how you, on a certain date,
may instruct The Bank of New York to vote the shares or other deposited
securities underlying your ADRs as you direct. For instructions to be valid,
The
Bank of New York must receive them on or before the date specified. The Bank
of
New York will try, as far as practical, subject to Israeli law and the
provisions of our Articles of Association, to vote or to have its agents vote
the shares or other deposited securities as you instruct. The Bank of New York
will only vote or attempt to vote as you instruct. However, if The Bank of
New
York does not receive your voting instructions, it will deem you to have
instructed it to give a discretionary proxy to vote the shares underlying your
ADRs to a person designated by us provided that no such instruction shall be
deemed given and no such discretionary proxy shall be given with respect to
any
matter as to which we inform The Bank of New York that (x) we do not wish such
proxy given, (y) substantial opposition exists, (z) such matter materially
affects the rights of the holders of the shares underlying the
ADRs.
We
cannot
assure you that you will receive the voting materials in time to ensure that
you
can instruct The Bank of New York to vote your shares. In addition, The Bank
of
New York and its agents are not responsible for failing to carry out voting
instructions or for the manner of carrying out voting instructions. This means
that you may not be able to exercise your right to vote and there may be nothing
you can do if your shares are not voted as you requested.
Rights
of Non-Israeli Shareholders to Vote
Our
ADSs
may be freely held and traded pursuant to the General Permit and the Currency
Control Law. The ownership or voting of ADSs by non-residents of Israel are
not
restricted in any way by our Articles of Association or by the laws of the
State
of Israel.
Fees
and Expenses
|
ADR
holders must pay:
|
For:
|
|
|
$5.00
(or less) per 100 ADSs
(or
portion thereof)
|
Each
issuance of an ADS, including as a result of a distribution of shares
or
rights or other property.
Each
cancellation of an ADS, including if the agreement
terminates.
|
|
|
$0.02
(or less) per ADS
|
Any
cash payment.
|
|
|
Registration
or Transfer Fees
|
Transfer
and registration of shares on the share register of the Foreign Registrar
from your name to the name of The Bank of New York or its agent when
you
deposit or withdraw shares.
|
|
|
Expenses
of The Bank of New York
|
Conversion
of foreign currency to U.S. dollars.
Cable,
telex and facsimile transmission expenses.
Servicing
of shares or deposited securities.
|
|
|
$0.02
(or less) per ADS per calendar year (if the depositary has not collected
any cash distribution fee during that year)
|
Depositary
services.
|
|
|
Taxes
and other governmental charges
|
As
necessary The Bank of New York or the Custodian have to pay on any
ADR or
share underlying an ADR, for example, stock transfer taxes, stamp
duty or
withholding taxes.
|
|
|
A
fee equivalent to the fee that would be payable if securities distributed
to you had been ordinary shares and the ordinary shares had been
deposited
for issuance of ADSs
|
Distribution
of securities distributed to holders of deposited securities which
are
distributed by the depositary to ADR
holders.
|
Payment
of Taxes
You
will
be responsible for any taxes or other governmental charges payable on your
ADRs
or on the deposited securities underlying your ADRs. The Bank of New York may
refuse to transfer your ADRs or allow you to withdraw the deposited securities
underlying your ADRs until such taxes or other charges are paid. It may apply
payments owed to you or sell deposited securities underlying your ADRs to pay
any taxes owed and you will remain liable for any deficiency. If it sells
deposited securities, it will, if appropriate, reduce the number of ADRs to
reflect the sale and pay to you any proceeds, or send to you any property,
remaining after it has paid the taxes.
Reclassifications,
Recapitalizations and Mergers
|
If
we:
|
Then:
|
|
|
Change
the nominal or par value of our shares; Reclassify, split up or
consolidate any of the deposited securities;
|
The
cash, shares or other securities received by The Bank of New York
will
become deposited securities. Each ADR will automatically represent
its
equal share of the new deposited securities. The Bank of New York
may, and
will if we ask it to, distribute some or all of the cash, shares
or other
securities it received. It may also issue new ADRs or ask you to
surrender
your outstanding ADRs in exchange for new ADRs, identifying the new
deposited securities.
|
|
|
Distribute
securities on the shares that are not distributed to you;
or
|
||
|
Recapitalize,
reorganize, merge, liquidate, sell all or substantially all of
our
assets, or takes any similar action.
|
Amendment
and Termination
We
may
agree with The Bank of New York to amend the agreement and the ADRs without
your
consent for any reason. If the amendment adds or increases fees or charges,
except for taxes and other governmental charges or registration fees, cable,
telex or facsimile transmission costs, delivery costs or other such expenses,
or
prejudices an important right of ADR holders, it will only become effective
thirty days after The Bank of New York notifies you of the amendment. At the
time an amendment becomes effective, you are considered, by continuing to hold
your ADR, to agree to the amendment and to be bound by the ADRs and the
agreement is amended.
The
Bank
of New York will terminate the agreement if we ask it to do so. The Bank of
New
York may also terminate the agreement if The Bank of New York has told us that
it would like to resign and we have not appointed a new depositary bank within
ninety days. In both cases, The Bank of New York must notify you at least ninety
days before termination.
After
termination, The Bank of New York and its agents will be required to do only
the
following under the agreement: (1) advise you that the agreement is terminated,
and (2) collect distributions on the deposited securities and deliver shares
and
other deposited securities upon cancellation of ADRs. After termination, The
Bank of New York will, if practical, sell any remaining deposited securities
by
public or private sale. After that, The Bank of New York will hold the proceeds
of the sale, as well as any other cash it is holding under the agreement for
the
pro rata benefit of the ADR holders that have not surrendered their ADRs. It
will not invest the money and will have no liability for interest. The Bank
of
New York's only obligations will be to account for the proceeds of the sale
and
other cash. After termination our only obligations will be with respect to
indemnification and to pay certain amounts to The Bank of New York.
Limitations
on Obligations and Liability to ADR Holders
The
agreement expressly limits our obligations and the obligations of The Bank
of
New York, and it limits our liability and the liability of The Bank of New
York.
We and The Bank of New York:
|
·
|
are
only obligated to take the actions specifically set forth in
the agreement
without negligence or bad faith;
|
|
·
|
are
not liable if either is prevented or delayed by law or circumstances
beyond their control from performing their obligations under
the
agreement;
|
|
·
|
are
not liable if either exercises discretion permitted under the
agreement;
|
|
·
|
have
no obligation to become involved in a lawsuit or other proceeding
related
to the ADRs or the agreement on your behalf or on behalf of any
other
party; and
|
|
·
|
may
rely upon any documents they believe in good faith to be genuine
and to
have been signed or presented by the proper
party.
|
In
the
agreement, we and The Bank of New York agree to indemnify each other under
certain circumstances.
84
Requirements
for Depositary Actions
Before
The Bank of New York will issue or register transfer of an ADR, make a
distribution on an ADR, or make a withdrawal of shares, The Bank of New York
may
require:
|
·
|
payment
of stock transfer or other taxes or other governmental charges
and
transfer or registration fees charged by third parties for
the
|
|
·
|
transfer
of any shares or other deposited
securities;
|
|
·
|
production
of satisfactory proof of the identity and genuineness of any signature
or
other information it deems necessary,
and
|
|
·
|
compliance
with regulations it may establish, from time to time, consistent
with the
agreement, including presentation of transfer
documents.
|
The
Bank
of New York may refuse to deliver, transfer, or register transfers of ADRs
generally when the books of The Bank of New York or our books are closed, or
at
any time if The Bank of New York or we think it advisable to do so. You have
the
right to cancel your ADRs and withdraw the underlying shares at any time
except:
|
·
|
when
temporary delays arise because: (1) The Bank of New York or we
have closed
its transfer books; (2) the transfer of shares is blocked to
permit voting
at a shareholders' meeting; or (3) we are paying a dividend on
the shares;
or
|
| · | when it is necessary to prohibit withdrawals in order to comply with any laws or governmental regulations that apply to ADRs or to the withdrawal of shares or other deposited securities. |
This
right of withdrawal may not be limited by any other provision of the
agreement.
Pre-Release
of ADRs
In
certain circumstances, subject to the provisions of the agreement, The Bank
of
New York may issue ADRs before deposit of the underlying shares. This is called
a pre-release of the ADR. The Bank of New York may also deliver shares upon
cancellation of pre-released ADRs (even if the ADRs are cancelled before the
pre-release transaction has been closed out). A pre-release is closed out as
soon as the underlying shares are delivered to The Bank of New York. The Bank
of
New York may receive ADRs instead of shares to close out a pre-release. The
Bank
of New York may pre-release ADRs only under the following conditions: (1) before
or at the time of the pre-release, the person to whom the pre-release is being
made must represent to The Bank of New York in writing that it or its customer
owns the shares or ADRs to be deposited; (2) the pre-release must be fully
collateralized with cash or other collateral that The Bank of New York considers
appropriate; and (3) The Bank of New York must be able to close out the
pre-release on not more than five business days' notice. In addition, The Bank
of New York will limit the number of ADRs that may be outstanding at any time
as
a result of prerelease, although The Bank of New York may disregard the limit
from time to time, if it thinks it is appropriate to do so.
Inspection
of Books of the Depositary
Under
the
terms of the agreement, holders of ADRs may inspect the transfer books of the
depositary at any reasonable time, provided, that such inspection shall not
be
for the purpose of communicating with holders of ADRs in the interest of a
business or object other than either our business or a matter related to the
deposit agreement or ADRs.
Book-Entry
Only Issuance - The Depository Trust Company
The
Depository Trust Company, or DTC, New York, New York, will act as securities
depository for the ADRs. The ADRs will be represented by one global security
that will be deposited with and registered in the name of Cede & Co. (DTC’s
partnership nominee), or such other name as may be requested by an authorized
representative of DTC. This means that we will not issue certificates to you
for
the ADRs. One global security will be issued to DTC, which will keep a
computerized record of its participants (for example, your broker) whose clients
have purchased the ADRs. Each participant will then keep a record of its
clients. Unless it is exchanged in whole or in part for a certificated security,
a global security may not be transferred. However, DTC, its nominees, and their
successors may transfer a global security as a whole to one another. Beneficial
interests in the global security will be shown on, and transfers of the global
security will be made only through, records maintained by DTC and its
participants.
DTC
is a
limited-purpose trust company organized under the New York Banking Law, a
“banking organization” within the meaning of the New York Banking Law, a member
of the United States Federal Reserve System, a “clearing corporation” within the
meaning of the New York Uniform Commercial Code and a “clearing agency”
registered under the provisions of Section 17A of the Exchange Act . DTC
holds securities that its participants (direct participants) deposit with DTC.
DTC also records the settlement among direct participants of securities
transactions, such as transfers and pledges, in deposited securities through
computerized records for direct participant’s accounts. This eliminates the need
to exchange certificates. Direct participants include securities brokers and
dealers, banks, trust companies, clearing corporations and certain other
organizations.
DTC’s
book-entry system is also used by other organizations such as securities brokers
and dealers, banks and trust companies that work through a direct participant.
The rules that apply to DTC and its participants are on file with the
SEC.
DTC
is a
wholly-owned subsidiary of The Depository Trust & Clearing Corporation, or
DTCC. DTCC is, in turn, owned by a number of DTC’s direct participants and by
the New York Stock Exchange, Inc., the American Stock Exchange, Inc.
and the National Association of Securities Dealers, Inc.
When
you
purchase ADRs through the DTC system, the purchases must be made by or through
a
direct participant, who will receive credit for the ADRs on DTC’s records. Since
you actually own the ADRs, you are the beneficial owner and your ownership
interest will only be recorded on the direct (or indirect) participants’
records. DTC has no knowledge of your individual ownership of the ADRs. DTC’s
records only show the identity of the direct participants and the amount of
ADRs
held by or through them. You will not receive a written confirmation of your
purchase or sale or any periodic account statement directly from DTC. You will
receive these from your direct (or indirect) participant. Thus the direct (or
indirect) participants are responsible for keeping accurate account of the
holdings of their customers like you.
We
will
wire dividend payments to DTC’s nominee, and we will treat DTC’s nominee as the
owner of the global security for all purposes. Accordingly, we will have no
direct responsibility or liability to pay amounts due on the global security
to
you or any other beneficial owners in the global security.
Any
redemption notices will be sent by us directly to DTC, who will in turn inform
the direct participants, who will then contact you as a beneficial
holder.
It
is
DTC’s current practice, upon receipt of any payment of dividends or liquidation
amount, to credit direct participants’ accounts on the payment date based on
their holdings of beneficial interests in the global securities as shown on
DTC’s records. In addition, it is DTC’s current practice to assign any
consenting or voting rights to direct participants whose accounts are credited
with preferred securities on a record date, by using an omnibus proxy. Payments
by participants to owners of beneficial interests in the global securities,
and
voting by participants, will be based on the customary practices between the
participants and owners of beneficial interests, as is the case with the ADRs
held for the account of customers registered in “street name.” However, payments
will be the responsibility of the participants and not of DTC or
us.
ADRs
represented by a global security will be exchangeable for certificated
securities with the same terms in authorized denominations only if:
|
·
|
DTC
is unwilling or unable to continue as depositary or if DTC ceases
to be a
clearing agency registered under applicable law and a successor depositary
is not appointed by us within 90 days; or
|
|
·
|
we
determine not to require all of the ADRs to be represented by a global
security.
|
If
the
book-entry only system is discontinued, the transfer agent will keep the
registration books for the ADRs at its corporate office.
The
information in this section concerning DTC and DTC’s book-entry system has been
obtained from sources we believe to be reliable, but we take no responsibility
for the accuracy thereof.
We
did
not have any transactions or loans with related parties during the fiscal
years
ended December 31, 2005, 2004 and 2003, or the during the fiscal quarter
ended
March 31, 2006.
Consolidated
Statements and Other Financial Information
Our
audited consolidated financial statements are included on pages F-1 through
F-41 of this registration statement. The consolidated financial statements
of
audited VivoQuest, Inc. are included on pages F-43 through F-77 of this
registration statement.
Significant
Changes
In
January 2006, Ron Bentsur was appointed Chief Executive Officer of XTLbio.
Mr.
Bentsur has nearly a decade of experience in the biotech industry. From June
2003 to February 2006, Mr. Bentsur served as Vice President, Finance and
Investor Relations of Keryx Biopharmaceuticals, Inc.. From October 2000 to
June
2003, Mr. Bentsur served as Director of Investor Relations at Keryx. From July
1998 to October 2000, he served as Director of Technology Investment Banking
at
Leumi Underwriters, where he was responsible for all technology/biotechnology
private placement and advisory transactions. From June 1994 to July 1998, Mr.
Bentsur worked as an investment banker at ING Barings Furman Selz. Mr. Bentsur
holds a B.A. in Economics and Business Administration with distinction from
the
Hebrew University of Jerusalem, Israel and an M.B.A., Magna Cum Laude, from
New
York University’s Stern Graduate School of Business.
In
March
2006, our board of directors granted our Chief Executive Officer options to
purchase a total of 7,000,000 ordinary shares at an exercise price equal to
$0.774 per share (closing price of the last trading day prior to official
appointment). These options are exercisable for a period of ten years from
the
date of issuance, and granted under the same terms and conditions as the 2001
Plan and any option agreement entered into with Mr. Bentsur. Of these,
2,333,334 options shall vest as follows: 777,782 options on the one-year
anniversary of the issuance of the options and 194,444 options at the end of
each quarter thereafter for the following two years. The balance of options
shall vest upon achievement of certain milestones (2,333,333 upon the
achievement of $350 million market capitalization or $75 million in working
capital, as set out in the agreement and 2,333,333 upon the achievement of
$550
million market capitalization or $125 million in working capital, as set out
in
the agreement).
In
March
2006, the board of directors also approved grants of a total of 9,898,719
options to our Chairman and 750,000 options to one of our non-executive
directors. These options are exercisable at an exercise price which is the
volume weighted average price per share of the ADRs on NASDAQ during the thirty
trading days prior to the board of directors’ approval divided by ten, $0.713.
The options shall vest as follows: (i) 1/3 of such options shall vest over
three
years, of which amounts, 1/3 shall vest and be exercisable upon the first
anniversary of the issuance of the options and the remainder shall vest and
be
exercisable on a quarterly basis; (ii) 1/3 of such options shall vest and be
exercisable upon our achieving a total market capitalization on a fully diluted
basis of more than US $350 million; and (iii) 1/3 of such options shall vest
upon our achieving a total market capitalization on a fully diluted basis of
more than US $550 million. The options can be exercised for a period of ten
years. The grant of such options is conditional upon approval of the
shareholders at a duly convened shareholder meeting expected to take place
later
this year.
On
March
22, 2006, we completed a private placement of 46,666,670 ordinary shares
(equivalent to 4,666,667 ADRs) at $0.60 per share ($6.00 per ADR), together
with
warrants for the purchase of an aggregate of 23,333,335 ordinary shares
(equivalent to 2,333,333.5 ADRs) at an exercise price of $0.875 ($8.75 per
ADR),
for an aggregate consideration of approximately $28 million in gross proceeds.
See “Recent Developments.”
The
following discussion of Israeli and United States tax consequences material
to
our shareholders is not intended and should not be construed as legal or
professional tax advice and does not exhaust all possible tax considerations.
To
the extent that the discussion is based on new tax legislation, which has not
been subject to judicial or administrative interpretation, the views expressed
in the discussion might not be accepted by the tax authorities in question.
This
summary does not purport to be a complete analysis of all potential tax
consequences of owning ordinary shares or ADRs. In particular, this discussion
does not take into account the specific circumstances of any particular investor
(such as tax-exempt entities, certain financial companies, broker-dealers,
investors subject to Alternative Minimum Tax, investors that actually or
constructively own 10% or more of our voting securities, investors that hold
ordinary shares or ADRs as part of straddle or hedging or conversion
transaction, traders in securities that elect mark to market, banks and other
financial institutions or investors whose functional currency is not the U.S.
dollar), some of which may be subject to special rules.
We
urge shareholders and prospective purchasers of our ordinary shares and ADRs
to
consult their own tax advisors as to the U.S., Israeli, or other tax
consequences of the purchase, ownership and disposition of ordinary shares
and
ADRs, including, in particular, the effect of any foreign, state or local
taxes.
Israeli
Tax Considerations
The
following discussion refers to the current tax law applicable to companies
in
Israel, with special reference to its effect on us. This discussion also
includes specified Israeli tax consequences to holders of our ordinary shares
and Israeli Government programs benefiting us.
Tax
Reforms
On
January 1, 2003 a comprehensive tax reform took effect in Israel (the Law for
Amendment of the Income Tax Ordinance (Amendment No. 132), 5762-2002, as
amended) (which we refer to as “the 2003 Reform”). Pursuant to the 2003 Reform,
resident companies are subject to Israeli tax on income on a worldwide basis.
In
addition, the concept of controlled foreign corporation was introduced according
to which an Israeli company may become subject to Israeli taxes on certain
income of a non-Israeli subsidiary if the subsidiary’s primary source of income
is passive income (such as interest, dividends, royalties, rental income or
certain capital gains). An Israeli company that is subject to Israeli taxes
on
the income of its non-Israeli subsidiaries will receive a credit for income
tax
paid by the subsidiary in its country of resident subject to certain
limitations. The 2003 Reform also substantially changed the system of taxation
of capital gains.
On
July
25, 2005 an additional tax reform took effect in Israel (the Law for Amendment
of the Income Tax Ordinance (Amendment No. 147) (which we refer to as “the 2005
Reform”). In general terms, pursuant to the 2005 Reform, and generally effective
from January 1, 2006, the Israeli corporate tax rates were and will be further
reduced, the capital gains tax rate that applies to Israeli individuals on
the
disposition of traded securities was increased and the tax rates that apply
to
dividends distributed by an Israeli company was partly reduced.
Corporate
Tax Rate
The
regular tax rate in Israel in 2006 is 31%. This rate is currently scheduled
to
decrease as follows: in 2007 - 29%, 2008 - 27%, 2009 - 26%, 2010 and after
-
25%”. However, the effective tax rate of a company which derives income from an
approved enterprise may be considerably less, as further discussed
below.
Tax
Benefits Under the Law for the Encouragement of Capital Investments,
1959
The
Law
for the Encouragement of Capital Investment, 1959, as amended, commonly referred
to as the Investment Law, provides that a proposed capital investment in
eligible facilities may, upon application to the Investment Center of the
Ministry of Industry and Trade of the State of Israel, be designated as an
Approved Enterprise. Each certificate of approval for an Approved Enterprise
relates to a specific investment program delineated both by its financial scope,
including its capital sources, and by its physical characteristics, for example,
the equipment to be purchased and utilized under the program. The tax benefits
derived from any certificate of approval relate only to taxable income
attributable to the specific Approved Enterprise. If a company has more than
one
approval or only a portion of its capital investments is approved, its effective
tax rate is the result of a weighted average of the applicable
rates.
Taxable
income of a company derived from an Approved Enterprise is subject to company
tax at the maximum rate of 25% rather than the usual rate in 2006 of 31% (as
mentioned above, gradually scheduled to be reduced to 25% in 2010), for the
benefit period. This period is ordinarily seven years, or ten years if the
company qualifies as a foreign investors’ company as described below, commencing
with the year in which the Approved Enterprise first generates taxable income.
However, this period is limited to 12 years from commencement of production
of
the Approved Enterprise or 14 years from the date of approval, whichever is
earlier.
A
company
that has been granted the status of an Approved Enterprise may elect to forego
entitlement to grants otherwise available for an Approved Enterprise, in return
for an alternative package of benefits. Under the alternative package of
benefits, a company’s undistributed income derived from an Approved Enterprise
will be exempt from company tax for a period of between two and ten years from
the first year of taxable income, depending on the geographic location of the
Approved Enterprise within Israel, and the company will be eligible for a
reduced tax rate for the remainder of the benefits period.
A
company
that has elected the alternative package of benefits and that subsequently
pays
a dividend out of income derived from the approved enterprise during the tax
exemption period will be subject to tax on the amount distributed, including
any
company tax on these amounts, at the rate which would have been applicable
had
it not elected the alternative package of benefits, generally 10%-25%, depending
on the percentage of the company’s shares held by foreign shareholders. The
dividend recipient is taxed at the reduced rate applicable to dividends from
approved enterprises, which is 15%, if the dividend is distributed during the
tax exemption period or within 12 years after this period, or in the case of
a
foreign investors’ company, without time limitation. The company must withhold
this tax at source, regardless of whether the dividend is converted into or
paid
in foreign currency.
A
company
that has an Approved Enterprise program is eligible for enhanced tax benefits
if
it qualifies as a foreign investors’ company. A foreign investors' company is a
company more than 25% of whose share capital and combined share and loan capital
is owned by non-Israeli residents. A company which qualifies as a foreign
investors' company and has an Approved Enterprise program is eligible for tax
benefits for a ten-year benefit period. The company tax rate applicable to
income earned from approved enterprise programs in the benefit period by a
company meeting these qualifications is as follows:
|
For
a company with foreign investment of
|
Company
tax rate
|
|||
|
More
than 25% and less than 49%
|
25%
|
|
||
|
49%
or more and less than 74%
|
20%
|
|
||
|
74%
or more and less than 90%
|
15%
|
|
||
|
90%
or more
|
10%
|
|
||
The
determination of foreign ownership is made on the basis of the lowest level
of
foreign ownership during the tax year.
Subject
to applicable provisions concerning income under the alternative package of
benefits, all dividends are considered to be attributable to the entire
enterprise and their effective tax rate is the result of a weighted average
of
the various applicable tax rates. Under the Investment Law, a company that
has
elected the alternative package of benefits is not obliged to attribute part
of
the dividend to exempt profits, and may generally decide from which year's
profits to declare dividends. We currently intend to reinvest any income derived
from our Approved Enterprise programs and not to distribute the income as a
dividend.
The
Investment Center bases its decision whether or not to approve an application
on
the criteria set forth in the Investment Law and regulations and the then
prevailing policy of the Investment Center. In addition, the benefits available
to an Approved Enterprise are conditioned upon the fulfillment of conditions
stipulated in the Investment Law and its regulations and in the criteria in
the
specific certificate of approval, as described above. If a company does not
meet
these conditions, it would be required to refund the amount of tax benefits,
together with consumer price index linkage adjustment and interest.
Additionally
after receiving the certificate of approval from the Investment Center, a
company must meet certain reporting requirements. The company must file periodic
audited reports on the progress in implementing the program. Additionally,
where
a company has completed the implementation of investing in fixed assets, a
final
implementation report must be filed with, and reviewed by, the Investment
Center. Should the Investment Center determine that the investments in assets
were made in accordance with the certificate of approval and that the required
minimum capital has been invested, it will issue a final approval of
implementation, which will also indicate the year that will be the first year
of
potential benefits under the Approved Enterprise.
On
March
29, 2005, the Israeli Parliament enacted an amendment to the Investment Law,
which is intended to provide expanded tax benefits to local and foreign
investors and to simplify the bureaucratic process relating to approval of
investments qualifying under the Investment Law.
The
amendment to the Investment Law does not retroactively apply for investment
programs having an Approved Enterprise approval certificate from the Investment
Center issued up to December 31, 2004 (even when investments under these
programs are conducted after January 1, 2005). Consequently, the amendment
to
the Investment Law should not impact an existing Approved Enterprise, that
received an approval certificate prior to December 2004. The new tax regime
will
only apply to a for a new Approved Enterprise and to an Approved Enterprise
expansion for which the first year of benefits was 2004 or later.
Under
the
amended Investment Law, if an investment project meets all of the eligibility
criteria under the alternative benefits route as set forth in the amended
Investment Law and in regulations to be issued thereunder, such project will
automatically qualify for the Approved Enterprise taxation benefits under the
alternative package of benefits with no need for prior approval from the Israeli
Tax Authorities. In addition, the amended Investment Law provides that the
criteria for conferral of tax benefits in the alternative package of benefits
of
the Investment Law be handled by the Israeli Tax Authorities rather than the
Investment Center. In this respect a mechanism will be available which will
enable a company to apply for a pre-ruling from the Israeli Tax Authorities
to
obtain certainty as to the investment taxation status of its investment under
the amended Investment Law.
The
Investment Center has granted us Approved Enterprise status, which approval
was
granted prior to December 31, 2004, and is therefore entitled to the benefits
afforded by the Investment Law prior to its amendment. Accordingly, our
undistributed taxable income derived from this program will be tax exempt for
a
period of two years beginning with the year in which we first generate taxable
income, and thereafter will be subject to a reduced tax rate of 25% or less,
if
we qualify as a foreign investors' company, for a period of between five and
eight years, depending on the percentage of our capital held by non-Israeli
shareholders. However, this benefit period cannot extend beyond 12 years from
the year of commencement of operations or 14 years from the year in which
approval was granted, whichever is earlier. To date, we have not generated
taxable income.
To
date,
the Investment Center is still reviewing our final implementation report, and
as
a result, we have not yet received final implementation approval with respect
to
our Approved Enterprise from the Investment Center. Additionally, given our
significant amount of net operating losses, and the limitation mentioned above
to the benefit period, there is no certainty if and when we would be able to
enjoy the tax benefits described above.
Tax
Benefits for Research and Development
Israeli
tax law allows, under specific conditions, a tax deduction in the year incurred
for expenditures, including capital expenditures, relating to scientific
research and development projects, if the expenditures are approved by the
relevant Israeli government ministry, determined by the field of research,
and
the research and development is for the promotion of the company and is carried
out by or on behalf of the company seeking the deduction. Expenditures not
so
approved are deductible over a three-year period. Expenditures made out of
proceeds made available to us through government grants are automatically
deducted during a one year period.
Tax
Benefits Under the Law for the Encouragement of Industry (Taxes),
1969
The
Law
for the Encouragement of Industry (Taxes), 1969, generally referred to as the
Industry Encouragement Law, provides several tax benefits for industrial
companies. An industrial company is defined as a company resident in Israel,
at
least 90% of the income of which in a given tax year exclusive of income from
specified government loans, capital gains, interest and dividends, is derived
from an industrial enterprise owned by it. An industrial enterprise is defined
as an enterprise whose major activity in a given tax year is industrial
production activity.
Under
the
Industry Encouragement Law, industrial companies are entitled to a number of
corporate tax benefits, including:
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deduction
of purchase of know-how and patents over an eight-year period;
and
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the
right to elect, under specified conditions, to file a consolidated
tax
return with additional related Israeli industrial companies and an
industrial holding company.
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Under
some tax laws and regulations, an industrial enterprise may be eligible for
special depreciation rates for machinery, equipment and buildings. These rates
differ based on various factors, including the date the operations begin and
the
number of work shifts. An industrial company owning an approved enterprise
may
choose between these special depreciation rates and the depreciation rates
available to the approved enterprise.
Eligibility
for benefits under the Industry Encouragement Law is not subject to receipt
of
prior approval from any governmental authority.
We
believe that we currently qualify as an industrial company within the definition
of the Industry Encouragement Law. We cannot assure you that the Israeli tax
authorities will agree that we qualify, or, if we qualify, that we will continue
to qualify as an industrial company or that the benefits described above will
be
available to us in the future.
Special
Provisions Relating to Taxation under Inflationary
Conditions
The
Income Tax Law (Inflationary Adjustments), 1985, generally referred to as the
Inflationary Adjustments Law, represents an attempt to overcome the problems
presented to a traditional tax system by an economy undergoing rapid inflation.
The Inflationary Adjustments Law is highly complex. Its features, which are
material to us, can be described as follows:
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where
a company's equity, as defined in the law, exceeds the cost of fixed
assets as defined in the Inflationary Adjustments Law, a deduction
from
taxable income that takes into account the effect of the applicable
annual
rate of inflation on the excess is allowed up to a ceiling of 70%
of
taxable income in any single tax year, with the unused portion permitted
to be carried forward on a linked basis. If the cost of fixed assets,
as
defined in the Inflationary Adjustments Law, exceeds a company's
equity,
then the excess multiplied by the applicable annual rate of inflation
is
added to taxable income;
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subject
to specified limitations, depreciation deductions on fixed assets
and
losses carried forward are adjusted for inflation based on the increase
in
the consumer price index; and
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Israeli
Estate and Gift Taxes
Generally,
Israel does not currently impose taxes on inheritance or bona fide gifts. For
transfer of assets by inheritance or gift that would normally be subject to
capital gains tax or land appreciation tax, the recipient’s tax cost basis and
date of purchase are generally deemed to be the same as those for the transferor
of the property.
Capital
Gains Tax on Sale of our Ordinary Shares by Both Residents and Non-Residents
of
Israel
Israeli
law generally imposes a capital gains tax on the sale of capital assets located
in Israel, including shares in Israeli resident companies, by both residents
and
non-residents of Israel, unless a specific exemption is available or unless
a
treaty between Israel and the country of the non-resident provides otherwise.
The law distinguishes between the inflationary surplus and the real gain. The
inflationary surplus is the portion of the total capital gain, which is
equivalent to the increase of the relevant asset’s purchase price attributable
to the increase in the Israeli consumer price index from the date of purchase
to
the date of sale. The real gain is the excess of the total capital gain over
the
inflationary surplus. A non resident that invests in taxable assets with foreign
currency may elect to calculate the inflationary amount by using such foreign
currency.
Non-Israeli
residents will be exempt from Israeli capital gains tax on any gains derived
from the sale of shares publicly traded on a stock exchange recognized by the
Israeli Ministry of Finance (including the Tel-Aviv Stock Exchange and Nasdaq),
provided such shareholders did not acquire their shares prior to an initial
public offering and that such capital gains are not derived by a permanent
establishment of the foreign resident in Israel. Notwithstanding the foregoing,
dealers in securities in Israel are taxed at the regular tax rates applicable
to
business income. However, Non-Israeli corporations will not be entitled to
such
exemption if an Israeli resident (1) has a controlling interest of 25% or more
in such non-Israeli corporation, or (2) is the beneficiary of, or is entitled
to, 25% or more of the revenue or profits of such non-Israeli corporation,
whether directly or indirectly. In any event, the provisions of the tax reform
shall not affect the exemption from capital gains tax for gains accrued before
January 1, 2003, as described in the previous paragraph.
On
July
25, 2005, the 2005 Reform came into effect. Pursuant to the 2005 Reform,
effective January 1, 2006, the capital gains tax imposed on Israeli tax resident
individuals on the sale of securities is 20%. With respect to an Israeli tax
resident individual who is a “substantial shareholder” on the date of sale of
the securities or at any time during the 12 months preceding such sale, the
capital gains tax rate was increased to 25%. A “substantial shareholder” is
defined as someone who alone, or together with another person, holds, directly
or indirectly, at least 10 % in one or all of any of the means of control in
the
corporation. With respect to Israeli tax resident corporate investors, effective
January 1, 2006 capital gains tax at the regular corporate rate will be imposed
on such taxpayers on the sale of traded shares.
Other
provisions may apply to shareholders that acquired their ordinary shares in
XTL
prior to our recent private placement and / or prior to January 1,
2003.
In
addition, pursuant to the Convention Between the Government of the United States
of America and the Government of Israel with Respect to Taxes on Income, as
amended (the “United States- Israel Tax Treaty”), the sale, exchange or
disposition of ordinary shares by a person who qualifies as a resident of the
United States within the meaning of the United States-Israel Tax Treaty and
who
is entitled to claim the benefits afforded to such person by the United States-
Israel Tax Treaty (a “Treaty United States Resident”) generally will not be
subject to the Israeli capital gains tax unless such “Treaty United States
Resident” holds, directly or indirectly, shares representing 10% or more of our
voting power during any part of the twelve- month period preceding such sale,
exchange or disposition, subject to certain conditions or if the capital gains
from such sale are considered as business income attributable to a permanent
establishment of the U.S. resident in Israel. However, under the United
States-Israel Tax Treaty, such “Treaty United States Resident” would be
permitted to claim a credit for such taxes against the United States federal
income tax imposed with respect to such sale, exchange or disposition, subject
to the limitations in United States laws applicable to foreign tax credits.
Taxation
of Dividends
Non-residents
of Israel are subject to income tax on income accrued or derived from sources
in
Israel
Dividends
distributed by an Israeli company to Israeli tax resident individuals or to
non-Israeli residents are subject to a 25% tax to be withheld at source (15%
in
the case of dividends distributed from the taxable income attributable to an
Approved Enterprise), unless a lower rate is provided in a treaty between Israel
and the shareholder’s country of residence. Dividends distributed by an Israeli
company to another Israeli tax resident company are generally exempt, unless
such dividends are distributed from taxable income attributable to an Approved
Enterprise, in which case such dividends are taxed at a rate of 15%, or unless
such dividends are distributed from income that was not taxed in Israel, in
which case such dividends are taxed at a rate of 25%.
Pursuant
to the 2005 Reform, effective January 1, 2006, the tax rate imposed on dividends
distributed by an Israeli company to Israeli tax resident individuals or to
non-Israeli residents was reduced to a tax at a rate of 20%. With respect to
“substantial shareholders,” as defined above, the applicable tax rate remains
25%. The taxation of dividends distributed by an Israeli company to another
Israeli corporate tax resident remains unchanged.
In
any
case, dividends distributed from the taxable income attributable to an Approved
Enterprise, to both Israeli tax residents and non-Israeli residents remains
subject to a 15% tax rate.
Under
the
U.S.-Israel Tax Treaty, the maximum Israeli tax and withholding tax on dividends
paid to a holder of ordinary shares who is a resident of the United States
is
generally 25%, but is reduced to 12.5% if the dividends are paid to a
corporation that holds in excess of 10% of the voting rights of company during
the company’s taxable year preceding the distribution of the Dividend and the
portion of the company’s taxable year in which the dividend was distributed.
Dividends of an Israeli company derived from the income of an Approved
Enterprise will still be subject to a 15% dividend withholding tax; if the
dividend is attributable partly to income derived from an Approved Enterprise,
and partly to other sources of income, the withholding rate will be a blended
rate reflecting the relative portions of the two types of income. A non-resident
of Israel who has dividend income derived from or accrued in Israel, from which
tax was withheld at the source, is generally exempt from the duty to file tax
returns in Israel in respect of such income, provided such income was not
derived from a business conducted in Israel by the taxpayer.
United
States Federal Income Tax Considerations
The
following discusses the material United States federal income tax consequences
to a holder of our ordinary shares who qualifies as a U.S. holder, which is
defined as:
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a
citizen or resident of the United States;
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a
corporation created or organized under the laws of the United States,
the
District of Columbia, or any state; or
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a
trust or estate, treated, for United States federal income tax purposes,
as a domestic trust or estate.
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This
opinion is based on current provisions of the Internal Revenue Code of 1986,
as
amended, which we refer to as the Code, current and proposed Treasury
regulations promulgated under the Code, and administrative and judicial
decisions as of the date of this prospectus, all of which are subject to change,
possibly on a retroactive basis. This opinion does not address any aspect of
state, local or non-U.S. tax laws. Further, this opinion does not purport to
be
a comprehensive description of all of the tax considerations that may be
relevant to U.S. holders entitled to special treatment under U.S. federal income
tax laws, for example, financial institutions, insurance companies, tax-exempt
organizations and broker/dealers, and it does not address all aspects of U.S.
federal income taxation that may be relevant to any particular shareholder
based
on the shareholder's individual circumstances. In particular, this opinion
does
not address the potential application of the alternative minimum tax, or the
special U.S. federal income tax rules applicable in special circumstances,
including to U.S. holders who:
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have
elected mark-to-market accounting;
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hold
our ordinary shares as part of a straddle, hedge or conversion transaction
with other investments;
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own
directly, indirectly or by attribution at least 10% of our voting
power;
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are
tax exempt entities;
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are
persons who acquire shares in connection with employment or other
performance of services; and
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have
a functional currency that is not the U.S.
dollar.
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Additionally,
this opinion does not consider the tax treatment of partnerships or persons
who
hold ordinary shares through a partnership or other pass-through entity or
the
possible application of U.S. federal gift or estate taxes. Material aspects
of
U.S. federal income tax relevant to a holder other than a U.S. holder are also
described below.
Taxation
of Dividends Paid on Ordinary Shares
A
U.S.
holder will be required to include in gross income as ordinary income the amount
of any distribution paid on ordinary shares, including any Israeli taxes
withheld from the amount paid, to the extent the distribution is paid out of
our
current or accumulated earnings and profits as determined for U.S. federal
income tax purposes. Distributions in excess of these earnings and profits
will
be applied against and will reduce the U.S. holder’s basis in the ordinary
shares and, to the extent in excess of this basis, will be treated as gain
from
the sale or exchange of ordinary shares.
Certain
dividend income may be eligible for a reduced rate of taxation. Dividend income
will be taxed to a non-corporate holder at the applicable long-term capital
gains rate if the dividend is received from a “qualified foreign corporation,”
and the shareholder of such foreign corporation holds such stock for more than
60 days during the 120 day period that begins on the date that is 60 days before
the ex-dividend date for the stock. The holding period is tolled for any days
on
which the shareholder has reduced his risk of loss. A “qualified foreign
corporation” is one that is eligible for the benefits of a comprehensive income
tax treaty with the United States. A foreign corporation will be treated as
qualified with respect to any dividend paid, if its stock is readily tradable
on
an established securities market. However, a foreign corporation will not be
treated as qualified if it is a Passive Foreign Investment Company (as discussed
below) for the year in which the dividend was paid or the preceding year.
Distributions of current or accumulated earnings and profits paid in foreign
currency to a U.S. holder will be includible in the income of a U.S. holder
in a
U.S. dollar amount calculated by reference to the exchange rate on the day
the
distribution is received. A U.S. holder that receives a foreign currency
distribution and converts the foreign currency into U.S. dollars subsequent
to
receipt will have foreign exchange gain or loss based on any appreciation or
depreciation in the value of the foreign currency against the U.S. dollar,
which
will generally be U.S. source ordinary income or loss.
As
described above, we will generally be required to withhold Israeli income tax
from any dividends paid to holders who are not resident in Israel. See “Israeli
Tax Considerations—Taxation of Non-Resident Holders of Shares.” If a U.S. holder
receives a dividend from us that is subject to Israeli withholding, the
following would apply:
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You
must include the gross amount of the dividend, not reduced by the
amount
of Israeli tax withheld, in your U.S. taxable income.
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You
may be able to claim the Israeli tax withheld as a foreign tax credit
against your U.S. income tax liability. However, to the extent that
25% or
more of our gross income from all sources was effectively connected
with
the conduct of a trade or business in the United States (or treated
as
effectively connected, with limited exceptions) for a three-year
period
ending with the close of the taxable year preceding the year in which
the
dividends are declared, a portion of this dividend will be treated
as U.S.
source income, possibly reducing the allowable foreign
tax.
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The
foreign tax credit is subject to significant and complex limitations.
Generally, the credit can offset only the part of your U.S. tax
attributable to your net foreign source passive income. Additional
special
rules currently apply to taxpayers predominantly engaged in the active
conduct of a banking, insurance, financing or similar business.
Additionally, if we pay dividends at a time when 50% or more of our
stock
is owned by U.S. persons, you may be required to treat the part of
the
dividend attributable to U.S. source earnings and profits as U.S.
source
income, possibly reducing the allowable credit, unless you elect
to
calculate your foreign tax credit separately with respect to XTLbio
dividends.
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A
U.S. holder will be denied a foreign tax credit with respect to Israeli
income tax withheld from dividends received on the ordinary shares
to the
extent the U.S. holder has not held the ordinary shares for at least
16
days of the 30-day period beginning on the date which is 15 days
before
the ex-dividend date or to the extent the U.S. holder is under an
obligation to make related payments with respect to substantially
similar
or related property. Any days during which a U.S. holder has substantially
diminished its risk of loss on the ordinary shares are not counted
toward
meeting the 16-day holding period required by the
statute.
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If
you do not elect to claim foreign taxes as a credit, you will be
entitled
to deduct the Israeli income tax withheld from your XTLbio dividends
in
determining your taxable income.
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Individuals
who do not claim itemized deductions, but instead utilize the standard
deduction, may not claim a deduction for the amount of the Israeli
income
taxes withheld.
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If
you are a U.S. corporation holding our stock, the general rule is
that you
cannot claim the dividends-received deduction with respect to our
dividends. There is an exception to this rule if you own at least
10% of
our ordinary shares (by vote or value) and certain conditions are
met,
including that we were not a PFIC during the period you have held
our
ordinary shares.
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Special
rules, described below, apply if we are a passive foreign investment
company.
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Taxation
of the Disposition of Ordinary Shares
Subject
to the description of the passive foreign investment company rules below, upon
the sale, exchange or other disposition of our ordinary shares, a U.S. holder
will recognize capital gain or loss in an amount equal to the difference between
the U.S. holder's basis in the ordinary shares, which is usually the cost of
these shares, and the amount realized on the disposition. Capital gain from
the
sale, exchange or other disposition of ordinary shares held more than one year
is long-term capital gain and is eligible for a reduced rate of taxation for
non-corporate holders. In general, gain realized by a U.S. holder on a sale,
exchange or other disposition of ordinary shares generally will be treated
as
U.S. source income for U.S. foreign tax credit purposes. A loss realized by
a
U.S. holder on the sale, exchange or other disposition of ordinary shares is
generally allocated to U.S. source income. However, regulations require the
loss
to be allocated to foreign source income to the extent certain dividends were
received by the taxpayer within the 24-month period preceding the date on which
the taxpayer recognized the loss. The deductibility of a loss realized on the
sale, exchange or other disposition of ordinary shares is subject to limitations
for both corporate and individual shareholders.
A
U.S.
holder that uses the cash method of accounting calculates the U.S. dollar value
of the proceeds received from a sale of ordinary shares as of the date that
the
sale settles, and will generally have no additional foreign currency gain or
loss on the sale, while a U.S. holder that uses the accrual method of accounting
is required to calculate the value of the proceeds of the sale as of the trade
date and may therefore realize foreign currency gain or loss, unless the U.S.
holder has elected to use the settlement date to determine its proceeds of
sale
for purposes of calculating this foreign currency gain or loss. In addition,
a
U.S. holder that receives foreign currency upon disposition of our ordinary
shares and converts the foreign currency into U.S. dollars subsequent to receipt
will have foreign exchange gain or loss based on any appreciation or
depreciation in the value of the foreign currency against the U.S. dollar,
which
will generally be U.S. source ordinary income or loss.
Tax
Consequences If We Are A Passive Foreign Investment
Company
Special
tax rules apply to the timing and character of income received by a U.S. holder
of a Passive Foreign Investment Company, or PFIC. We will be a PFIC if either
75% or more of our gross income in a tax year is passive income or the average
percentage of our assets (by value) that produce or are held for the production
of passive income is at least 50%. The U.S. Internal Revenue Service, or IRS,
has indicated that cash balances, even if held as working capital, are
considered to be assets that produce passive income. Therefore, any
determination of PFIC status will depend upon the sources of our income, and
the
relative values of passive and non- passive assets, including goodwill.
Furthermore, because the goodwill of a publicly-traded corporation such as
us is
largely a function of the trading price of its shares, the valuation of that
goodwill is subject to significant change throughout each year. An initial
determination that we are a PFIC will generally apply for subsequent years
(whether or not we meet the requirements for PFIC status in those years) with
respect to any U.S. holder at the time of such determination. A determination
as
to a corporation’s status as a PFIC must be made annually. We believe that we
were a PFIC for the taxable year ended December 31, 2003. We believe that we
were likely not a PFIC for the taxable years ended December 31, 2004 and 2005.
Although such a determination is fundamentally factual in nature and generally
cannot be made until the close of the applicable taxable year, based on our
current operations, we believe that there is a significant likelihood that
we
will be classified as a PFIC in the 2006 taxable year and possibly in subsequent
years.
If
we
were classified as a PFIC, a special tax regime would apply to both (a) any
“excess distribution” by us (generally, the U.S. holder's ratable share of
distributions in any year that are greater than 125% of the average annual
distributions received by such U.S. holder in the three preceding years or
its
holding period, if shorter) and (b) any gain realized on the sale or other
disposition of your ordinary shares. Under this special regime, any excess
distribution and realized gain would be treated as ordinary income and the
federal income tax on such ordinary income is determined under the following
steps: (i) the amount of the excess distribution or gain is allocated ratably
over the U.S. holder's holding period for our ordinary shares; (ii) tax is
determined for amounts allocated to the first year in the holding period in
which we were classified as a PFIC and all subsequent years (except the year
in
which the excess distribution was received or the sale occurred) by applying
the
highest applicable tax rate in effect in the year to which the income was
allocated; (iii) an interest charge is added to this tax calculated by applying
the underpayment interest rate to the tax for each year determined under the
preceding sentence from the due date of the income tax return for such year
to
the due date of the return for the year in which the excess distribution or
sale
occurs; and (iv) amounts allocated to a year prior to the first year in the
U.S.
holder’s holding period in which we were classified as a PFIC or to the year in
which the excess distribution or the sale occurred are taxed as ordinary income
and no interest charge applies.
A
U.S.
holder may generally avoid the special PFIC regime by electing to treat his
PFIC
shares as a “qualified electing fund.” If a U.S. holder elects to treat PFIC
shares as a qualified electing fund, also known as QEF Election, the U.S. holder
must include annually in gross income (for each year in which PFIC status is
met) his pro
rata
share of
the PFIC’s ordinary earnings and net capital gains, whether or not such amounts
are actually distributed to the U.S. holder.
A
U.S.
holder may make a QEF Election with respect to a PFIC for any taxable year
in
which s/he was a shareholder. A QEF Election is effective for the year in which
the election is made and all subsequent taxable years of the U.S. holder.
Procedures exist for both retroactive elections and the filing of protective
statements. A U.S. holder making the QEF Election must make the election on
or
before the due date, as extended, for the filing of the U.S. holder's income
tax
return for the first taxable year to which the election will apply.
A
U.S.
holder must make a QEF Election by completing Form 8621, Return by a
Shareholder of a Passive Foreign Investment Company or Qualified Electing Fund,
and attaching it to their U.S. federal income tax return, and must satisfy
additional filing requirements each year the election remains in effect. From
fiscal 2005, we plan to comply with the record-keeping and reporting
requirements that are a prerequisite to making a “qualified electing fund”
election. However, if meeting those record-keeping and reporting requirements
becomes onerous, we may decide, in our sole discretion, that such compliance
is
impractical and will so notify U.S. holders.
As
an
alternative to or in addition to the qualified electing fund election, a
so-called “mark-to- market” election may be made by a U.S. holder with respect
to ordinary shares owned at the close of such holder's taxable year, provided
that we are a PFIC and the ordinary shares are considered “marketable stock.”
The ordinary shares will be marketable stock if they are regularly traded on
a
national securities exchange that is registered with the Securities and Exchange
Commission, or the national market system established pursuant to section 11A
of
the Securities and Exchange Act of 1934, or an equivalent regulated and
supervised foreign securities exchange. If a U.S. holder were to make a
mark-to-market election with respect to ordinary shares, such holder generally
would include as ordinary income (or, to the extent of prior unreversed
inclusions, be allowed an ordinary loss deduction, as the case may be) an amount
equal to the difference between the fair market value of the holder's ordinary
shares as of the close of the holder's taxable year and its adjusted basis.
Gains from an actual sale or other disposition of the ordinary shares will
be
treated as ordinary income, and any losses incurred on an actual sale or other
disposition of the ordinary shares will be treated as ordinary loss to the
extent of any prior unreversed inclusions. The mark-to-market election is made
on a shareholder-by-shareholder basis and is effective for the taxable year
for
which made and all subsequent years until either (a) the ordinary shares cease
to be marketable stock or (b) the election is revoked with the consent of the
IRS.
A
U.S.
holder who did not make a QEF Election either to (i) treat us as a “qualified
electing fund,” or (ii) mark our ordinary shares and/or ADRs to market, will be
subject to the following:
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gain
recognized by the U.S. holder upon the disposition of, as well as
income
recognized upon receiving certain dividends on the ordinary shares
and/or
ADRs would be taxable as ordinary income;
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the
U.S. holder would be required to allocate such dividend income and/or
disposition gain ratably over such U.S. holder's entire holding period
for
such XTLbio ordinary shares and/or ADRs;
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the
amount allocated to each year other than the year of the dividend
payment
or disposition and pre-PFIC years would be subject to tax at the
highest
applicable tax rate, and an interest charge would be imposed with
respect
to the resulting tax liability;
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the
U.S. holder would be required to file an annual return on IRS Form
8621
regarding distributions received on, gain recognized on dispositions
of,
our ordinary shares and/or ADRs; and
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any
U.S. holder who acquired the ordinary shares and/or ADRs upon the
death of
the shareholder would not receive a step-up to market value of his
income
tax basis for such ordinary shares and/or ADRs. Instead such U.S.
holder
beneficiary would have a tax basis equal to the decedent's basis,
if
lower.
|
In
view of the complexity of the issues regarding our treatment as a PFIC, U.S.
shareholders are urged to consult their own tax advisors for guidance as to
our
status as a PFIC.
United
States Federal Income Tax Consequences for Non-U.S. holders of Ordinary
Shares
Except
as
described in "Information Reporting and Back-up Withholding" below, a Non-U.S.
holder of ordinary shares will not be subject to U.S. federal income or
withholding tax on the payment of dividends on, and the proceeds from the
disposition of, ordinary shares, unless:
|
·
|
the
item is effectively connected with the conduct by the Non-U.S. holder
of a
trade or business in the United States and, in the case of a resident
of a
country which has a tax treaty with the United States, the item is
attributable to a permanent establishment or, in the case of an
individual, a fixed place of business, in the United States;
|
|
·
|
the
Non-U.S. holder is subject to tax under the provisions of United
States
tax law applicable to U.S. expatriates; or
|
|
·
|
the
individual non-U.S. holder is present in the United States for 183
days or
more in the taxable year of the sale and certain other conditions
are
met.
|
Information
Reporting and Back-Up Withholding
U.S.
holders generally are subject to information reporting requirements with respect
to dividends paid in the United States on ordinary shares. Existing regulations
impose back-up withholding on dividends paid in the United States on ordinary
shares unless the U.S. holder provides IRS Form W-9 or otherwise establishes
an
exemption. U.S. holders are subject to information reporting and back-up
withholding at a rate of 28% on proceeds paid from the disposition of ordinary
shares unless the U.S. holder provides IRS Form W-9 or otherwise establishes
an
exemption.
Non-U.S.
holders generally are not subject to information reporting or back-up
withholding with respect to dividends paid on, or upon the disposition of,
ordinary shares, provided that the non-U.S. holder provides a taxpayer
identification number, certifies to its foreign status, or otherwise establishes
an exemption to the U.S. financial institution holding the ordinary shares.
Non
U.S. holders holding stock in a foreign corporation in a foreign bank or
financial institution have no U.S. reporting requirements.
Prospective
investors should consult their tax advisors concerning the effect, if any,
of
these Treasury regulations on an investment in ordinary shares. The amount
of
any back-up withholding will be allowed as a credit against a U.S. or Non-U.S.
holder's United States federal income tax liability and may entitle the Holder
to a refund, provided that specified required information is furnished to the
IRS on a timely basis.
United
States Federal Income Tax Consequences for XTLbio
The
residency of the Chairman of our Board of Directors and our Chief Executive
Officer in the United States, as well as other less significant contacts that
we
have with the United States, could lead to a determination by the U.S. Internal
Revenue Service that we have a “permanent establishment” in the United States
beginning in 2005. As a result, any income attributable to such U.S. permanent
establishment would be subject to U.S. corporate income tax in the same manner
as if we were a United States corporation. The maximum U.S. corporate income
tax
rate (not including applicable state and local tax rates) is currently at 35%.
In addition, if this occurred, we may be subject to an additional branch profits
tax of 30% on our U.S. effectively connected earnings and profits, subject
to
adjustment, for that taxable year if certain conditions occur, unless we qualify
for the reduced 12.5% U.S. branch profits tax rate pursuant to the United
States-Israel tax treaty. We would be potentially able to credit foreign taxes
against our U.S. tax liability in connection with income attributable to our
U.S. permanent establishment and subject to U.S. and foreign income
tax.
At
present, we do not earn any taxable income for U.S. tax purposes. If we do
eventually earn taxable income attributable to a U.S. permanent establishment,
we would be able to utilize accumulated loss carryforwards to offset such income
only if these carryforwards were attributable to the U.S. permanent
establishment. We may not be able to utilize any of the accumulated loss
carryforwards shown on our balance sheet at December 31, 2005, to offset any
such U.S. tax liability since such loss carryforwards were accumulated under
Israeli tax laws. U.S. corporate tax rates are higher than those to which we
are
subject in the State of Israel, and if we are subject to U.S. corporate tax,
it
would have a material adverse effect on our results of operations.
The
above comments are intended as a general guide to the current position. Any
person who is in any doubt as to his taxation position, and who requires more
detailed information than the general outline above or who is subject to tax
in
a jurisdiction other than the United States should consult his professional
advisers.
Our
legal
advisers are Alston & Bird LLP, 90 Park Avenue, New York, New York 10016,
United States of America and Kantor & Co., Oz House, 14 Abba Hilel Silver
(12th Floor), Ramat Gan 52506, State of Israel.
The
financial statements of XTL Biopharmaceuticals Ltd. as of December 31, 2005,
2004, and for each of the years in the three year period ended December 31
2005
and for the period from March 9, 1993 (inception) to December 31, 2005 included
in this prospectus on Form F−1 have been so included in reliance on the report
(which contains an explanatory paragraph relating to our ability to continue
as
a going concern as described in Note 1a(2) to the financial statements) of
Kesselman & Kesselman, a member of PricewaterhouseCoopers International
Ltd., an independent registered public accounting firm, Trade Tower, 25 Hamered
Street, Tel Aviv 68125, Israel, except with respect to the period from March
9,
1993 to December 31, 2000 which is included in reliance on the report of
Somekh
Chaikin a member firm of KPMG International, an independent registered public
accounting firm, KPMG Millennium Tower, 17 Ha'arba'a Street, Tel Aviv, 64739,
Israel, which reports appear elsewhere herein and upon the authority of said
firms as experts in auditing and accounting.
The
financial statements as of December 31, 2004 and for the year then ended
of
VivoQuest, Inc. ("VivoQuest") included in this Registration Statement have
been
audited by Cornick, Garber & Sandler, LLP, an independent registered public
accounting firm. Such financial statements have been so included in reliance
on
the report (which contains an explanatory paragraph related to VivoQuest's
ability to continue as a going concern as described in the notes to the
financial statements of VivoQuest) of such independent registered public
accounting firm given on the authority of such firm as experts in auditing
and
accounting.
The
statement of redeemable preferred stock and stockholders' deficiency of
VivoQuest, Inc. for the period from September 29, 1998 (inception) to December
31, 2003 included in this Registration Statement has been so included in
reliance on the report of PricewaterhouseCoopers LLP, independent accountants,
given on the authority of said firm as experts in auditing and
accounting.
We
have
filed with the SEC a registration statement on Form F-1 under the Securities
Act, with respect to our ADRs offered hereby. This prospectus, which forms
part
of the registration statement, does not contain all of the information set
forth
in the registration statement and the exhibits and schedules to the registration
statement. Some items are omitted in accordance with the rules and regulations
of the SEC. For further information about us and our ordinary shares and our
ADRs, we refer you to the registration statement and the exhibits and schedules
to the registration statement filed as part of the registration statement.
Statements contained in this prospectus as to the contents of any contract
or
other document filed as an exhibit are qualified in all respects by reference
to
the actual text of the exhibit. You may read and copy the registration
statement, including the exhibits and schedules to the registration statement,
at the SEC’s Public Reference Room at 100 F Street, N.E., Washington, D.C.
20549. You can obtain information on the operation of the Public Reference
Room
by calling the SEC at 1-800-SEC-0330. In addition, the SEC maintains an Internet
site at www.sec.gov,
from
which you can electronically access the registration statement, including the
exhibits and schedules to the registration statement.
XTL
BIOPHARMACEUTICALS LTD.
(A
Development Stage Company)
2005
ANNUAL REPORT
|
Page
|
|
|
F-2
|
|
|
F-4
|
|
|
F-5
|
|
|
F-6
|
|
|
F-10
|
|
|
F-12
|
F-1
To
the
Shareholders of
XTL
BIOPHARMACEUTICALS LTD.
(A
Development Stage Company)
We
have
audited the consolidated balance sheets of XTL Biopharmaceuticals Ltd.
(A Development Stage Company; hereafter - the "Company") and its subsidiary
as of December 31, 2005 and 2004 and the related consolidated statements of
operations, changes in shareholders' equity and cash flows for each of the
three
years ended December 31, 2005 and cumulatively for the period from January
1,
2001 to December 31, 2005 (see also below). These consolidated financial
statements are the responsibility of the Company's Board of Directors and
management. Our responsibility is to express an opinion on these consolidated
financial statements based on our audits. We did not audit the cumulative totals
of the Company for the period from March 9, 1993 (date of incorporation) to
December 31, 2000, which totals reflect a deficit of $25,201,000 accumulated
during the development stage. Those cumulative totals were audited by another
independent registered public accounting firm whose report, dated May 3, 2005,
expressed an unqualified opinion on the cumulative amounts through December
31,
2000. Our opinion, insofar as it relates to amounts included for that period
is
based on the report of the other independent registered public accounting firm,
mentioned above.
We
conducted our audits in accordance with the standards of the Public Company
Accounting Oversight Board (United States of America) and with auditing
standards generally accepted in Israel, including those prescribed by the
Israeli Auditors (Mode of Performance) Regulations, 1973. Those standards
require that we plan and perform the audit to obtain reasonable assurance about
whether the financial statements are free of material misstatement. An audit
includes examining, on a test basis, evidence supporting the amounts and
disclosures in the financial statements. An audit also includes assessing the
accounting principles used and significant estimates made by the Company’s Board
of Directors and management, as well as evaluating the overall financial
statement presentation. We believe that our audits and the report of other
independent registered public accounting firm provide a reasonable basis for
our
opinion.
In
our
opinion, based upon our audits and the report of the other independent
registered public accounting firm, the consolidated financial statements
referred to above, present fairly, in all material respects, the consolidated
financial position of the Company and its subsidiary as of December 31, 2005
and
2004, and the consolidated results of operations, changes in shareholders'
equity, and cash flows for each of the three years in the period ended
December 31, 2005 and for the cumulative period from March 9, 1993
(incorporation date) to December 31, 2005, in conformity with accounting
principles generally accepted in the United States of America.
The
financial statements have been prepared assuming that the Company will continue
as a going concern. As discussed in note 1a(2) to the financial statements,
the
Company incurred significant losses from operations and has an accumulated
deficit at December 31, 2005 which raise substantial doubt about the Company’s
ability to continue as a going concern. Management's plans in regard to these
matters are also described in Note 1a(2). The financial statements do not
include any adjustments that might result from the outcome of this
uncertainty.
As
discussed in note 1o to the financial statements, the Company adopted Statement
of Financial Accounting Standards No.123 (revised 2004), Share Based Payment,
effective January 1, 2005.
Kesselman
& Kesselman
Certified
Public Accountants (Israel)
A
Member
of PricewaterhouseCoopers International Limited
Tel-Aviv,
Israel
March
17,
2006
F-2
REPORT
OF INDEPENDENT REGISTERED PUBLIC ACCOUNTING FIRM
To
the
Board of Directors and Shareholders of XTL Biopharmaceuticals Ltd.
(A
Development Stage Company):
We
have
audited the accompanying consolidated statements of operations, changes in
shareholders' equity and comprehensive income, and cash flows of XTL
Biopharmaceuticals Ltd. (A Development Stage Company) (the "Company") and
its
subsidiary for the period from March 9, 1993 to December 31, 2000. These
consolidated financial statements are the responsibility of the Company's
management and of the Company's Board of Directors. Our responsibility is
to
express an opinion on these consolidated financial statements based on our
audits.
We
conducted our audits in accordance with the Standards of the Public Company
Accounting Oversight Board (United States). Those standards require that
we plan
and perform the audit to obtain reasonable assurance about whether the financial
statements are free of material misstatement. An audit includes examining,
on a
test basis, evidence supporting the amounts and disclosures in the financial
statements. An audit also includes assessing the accounting principles used
and
significant estimates made by management, as well as evaluating the overall
financial statement presentation. We believe that our audits provide a
reasonable basis for our opinion.
In
our
opinion, the consolidated financial statements referred to above present
fairly,
in all material respects, the consolidated results of operations of the Company
and its subsidiary and their cash flows for the period from March 9, 1993
to
December 31, 2000, in conformity with generally accepted accounting principles
in the United States of America.
Somekh
Chaikin
Certified
Public Accountants (Isr.)
A
member
firm of KPMG International
Tel-Aviv,
Israel
May
3,
2005
F-3
XTL
BIOPHARMACEUTICALS LTD.
(A
Development Stage Company)
(in
thousands of U.S. dollars)
|
December
31
|
|||||||
|
2005
|
2004
|
||||||
|
A
s s e t s
|
|||||||
|
CURRENT
ASSETS:
|
|||||||
|
Cash
and cash equivalents
|
13,360
|
12,788
|
|||||
|
Short-term
bank deposits
|
—
|
10,136
|
|||||
|
Accounts
receivable - trade
|
—
|
543
|
|||||
|
Accounts
receivable - other
|
431
|
306
|
|||||
|
T
o
t a l current assets
|
13,791
|
23,773
|
|||||
|
EMPLOYEE
SEVERANCE PAY FUNDS
|
449
|
830
|
|||||
|
RESTRICTED
LONG-TERM DEPOSIT
|
110
|
113
|
|||||
|
PROPERTY
AND EQUIPMENT, NET
|
762
|
908
|
|||||
|
INTANGIBLE
ASSETS, NET
|
39
|
—
|
|||||
|
T
o
t a l assets
|
15,151
|
25,624
|
|||||
|
Liabilities
and shareholders’ equity
|
|||||||
|
CURRENT
LIABILITIES:
|
|||||||
|
Accounts
payable and accruals
|
2,007
|
3,134
|
|||||
|
Deferred
gain
|
399
|
399
|
|||||
|
T
o
t a l current liabilities
|
2,406
|
3,533
|
|||||
|
LIABILITY
IN RESPECT OF EMPLOYEE
|
|||||||
|
SEVERANCE
OBLIGATIONS
|
695
|
1,291
|
|||||
|
DEFERRED
GAIN
|
798
|
1,198
|
|||||
|
COMMITMENTS
AND CONTINGENCIES (Note 7)
|
|||||||
|
T
o
t a l liabilities
|
3,899
|
6,022
|
|||||
|
SHAREHOLDERS’
EQUITY:
|
|||||||
|
Ordinary
shares of NIS 0.02 par value (authorized: 300,000,000
as
of December 31, 2005 and 2004; issued and outstanding:
173,180,441
as of December 31, 2005 and 168,079,196 as of
December
31, 2004)
|
864
|
841
|
|||||
|
Additional
paid in capital
|
110,179
|
104,537
|
|||||
|
Deficit
accumulated during the development stage
|
(99,791
|
)
|
(85,776
|
)
|
|||
|
T
o
t a l shareholders’ equity
|
11,252
|
19,602
|
|||||
|
T
o
t a l liabilities and shareholders’ equity
|
15,151
|
25,624
|
|||||
|
/s/
Michael Weiss
|
/s/
Ron Bentsur
|
|
|
Michael
Weiss
|
Ron
Bentsur
|
|
|
Chairman
of the Board of Directors
|
Chief
Executive Officer
|
|
Date
of
approval of the financial statements: March 17, 2006
The
accompanying notes are an integral part of the financial
statements.
F-4
XTL
BIOPHARMACEUTICALS LTD.
(A
Development Stage Company)
(in
thousands of U.S. dollars, except share and per share amounts)
|
Period
from
|
|||||||||||||
|
March
9, 1993*
|
|||||||||||||
|
Year
ended December 31
|
to
December 31,
|
||||||||||||
|
REVENUES:
|
2005
|
2004
|
2003
|
2005
|
|||||||||
|
Reimbursed
out-of-pockets expenses
|
2,743
|
3,269
|
—
|
6,012
|
|||||||||
|
License
|
454
|
185
|
—
|
639
|
|||||||||
|
3,197
|
3,454
|
—
|
6,651
|
||||||||||
|
COST
OF REVENUES:
|
|||||||||||||
|
Reimbursed
out-of-pockets expenses
|
2,743
|
3,269
|
—
|
6,012
|
|||||||||
|
License
(with respect to royalties)
|
54
|
32
|
—
|
86
|
|||||||||
|
2,797
|
3,301
|
—
|
6,098
|
||||||||||
|
GROSS
MARGIN
|
400
|
153
|
—
|
553
|
|||||||||
|
RESEARCH
AND DEVELOPMENT
|
|
||||||||||||
|
COSTS
(includes non-cash compensation
|
|||||||||||||
|
of
$112, $30 and $0, in 2005, 2004
|
|||||||||||||
|
and
2003, respectively)
|
7,313
|
11,985
|
14,022
|
82,890
|
|||||||||
|
L
E S S - PARTICIPATIONS
|
—
|
—
|
3,229
|
10,950
|
|||||||||
|
7,313
|
11,985
|
10,793
|
71,940
|
||||||||||
|
IN
- PROCESS RESEARCH AND
|
|||||||||||||
|
DEVELOPMENT
COSTS
|
1,783
|
—
|
—
|
1,783
|
|||||||||
|
GENERAL
AND ADMINISTRATIVE
|
|||||||||||||
|
EXPENSES
(includes non-cash
|
|||||||||||||
|
compensation
of $2,641, $2 and $0,
|
|||||||||||||
|
in
2005, 2004 and 2003, respectively)
|
5,457
|
4,134
|
3,105
|
29,012
|
|||||||||
|
BUSINESS
DEVELOPMENT COSTS
|
|||||||||||||
|
(includes
non-cash compensation of $10 in
|
|||||||||||||
|
2005,
and $0, in 2004 and 2003, respectively)
|
227
|
810
|
664
|
4,513
|
|||||||||
|
OPERATING
LOSS
|
14,380
|
16,776
|
14,562
|
106,695
|
|||||||||
|
FINANCIAL
INCOME -
net
|
443
|
352
|
352
|
7,143
|
|||||||||
|
LOSS
BEFORE INCOME TAXES
|
13,937
|
16,424
|
14,210
|
99,552
|
|||||||||
|
INCOME
TAXES
|
78
|
49
|
78
|
239
|
|||||||||
|
LOSS
FOR THE PERIOD
|
14,015
|
16,473
|
14,288
|
99,791
|
|||||||||
|
BASIC
AND DILUTED LOSS PER
|
|||||||||||||
|
ORDINARY
SHARE
|
$
|
0.08
|
$
|
0.12
|
$
|
0.13
|
|||||||
|
WEIGHTED
AVERAGE NUMBER OF
|
|||||||||||||
|
SHARES
USED IN COMPUTING BASIC
|
|||||||||||||
|
AND
DILUTED LOSS PER ORDINARY
|
|||||||||||||
|
SHARE
|
170,123,003
|
134,731,766
|
111,712,916
|
||||||||||
*
Incorporation date, see note 1a.
The
accompanying notes are an integral part of the financial
statements.
F-5
XTL
BIOPHARMACEUTICALS LTD.
(A
Development Stage Company)
(in
thousands of U.S. dollars, except share amounts)
|
Preferred
shares
|
Ordinary
shares
|
Additional
|
||||||||||||||
|
Number
of
|
Number
of
|
paid-in
|
||||||||||||||
|
shares
|
Amount
|
shares
|
Amount
|
capital
|
||||||||||||
|
CHANGES
DURING THE PERIOD
|
||||||||||||||||
|
FROM
MARCH 9, 1993 (DATE OF
|
||||||||||||||||
|
INCORPORATION)
TO
DECEMBER
31, 2002 :
|
||||||||||||||||
|
Comprehensive
loss:
|
||||||||||||||||
|
Loss
for the period
|
—
|
—
|
—
|
—
|
—
|
|||||||||||
|
Net
unrealized loss
|
—
|
—
|
—
|
—
|
—
|
|||||||||||
|
Comprehensive
loss
|
—
|
—
|
—
|
—
|
—
|
|||||||||||
|
Employee
stock options expenses
|
—
|
—
|
—
|
—
|
377
|
|||||||||||
|
Non-employee
stock option expenses
|
—
|
—
|
—
|
—
|
106
|
|||||||||||
|
Exercise
of share warrants in 2000
|
—
|
—
|
1,499,980
|
7
|
340
|
|||||||||||
|
Exercise
of share warrants in 2001
|
—
|
—
|
208,000
|
1
|
74
|
|||||||||||
|
Exercise
of employee stock
options
in 1999
|
15,600
|
**
|
—
|
—
|
**
|
|||||||||||
|
Exercise
of employee stock
options
in 2000
|
—
|
—
|
162,500
|
1
|
—
|
|||||||||||
|
Exercise
of employee stock
options
in 2001
|
—
|
—
|
59,138
|
**
|
26
|
|||||||||||
|
Exercise
of employee stock
options
in 2002
|
—
|
—
|
38,326
|
**
|
20
|
|||||||||||
|
Issuance
of share capital in 1993 (net
of
$912 - issuance expenses)
|
7,705,470
|
45
|
—
|
—
|
5,545
|
|||||||||||
|
Issuance
of share capital in 1994 (net
of
$22 - issuance expenses)
|
717,500
|
5
|
—
|
—
|
2,103
|
|||||||||||
|
Issuance
of share capital in 1996 (net
of
$646 - issuance expenses)
|
6,315,810
|
49
|
—
|
—
|
5,314
|
|||||||||||
|
Issuance
of share capital in 1998 (net
of
$1,650 - issuance expenses)
|
26,319,130
|
139
|
—
|
—
|
12,036
|
|||||||||||
|
Issuance
of share capital in 1999 (net
of
$49 - issuance expenses)
|
2,513,940
|
12
|
—
|
—
|
1,189
|
|||||||||||
|
Issuance
of share capital in 2000
|
—
|
—
|
15,183,590
|
75
|
16,627
|
|||||||||||
|
Bonus
shares
|
7,156,660
|
41
|
19,519,720
|
97
|
(138
|
)
|
||||||||||
|
Conversion
of preferred shares into
ordinary
shares
|
(50,744,110
|
)
|
(291
|
)
|
50,744,110
|
291
|
—
|
|||||||||
|
Receipts
in respect of share warrants
|
||||||||||||||||
|
(expired
in 1999)
|
—
|
—
|
—
|
—
|
89
|
|||||||||||
|
Initial
public offering (“IPO”) of the
|
||||||||||||||||
|
Company’s
shares under a prospectus
|
||||||||||||||||
|
dated
September 20, 2000 (net of
|
||||||||||||||||
|
$ 5,199-issuance
expenses)
|
—
|
—
|
23,750,000
|
118
|
45,595
|
|||||||||||
|
BALANCE
AT DECEMBER 31, 2002
|
—
|
—
|
111,165,364
|
590
|
89,303
|
|||||||||||
**
Represents an amount less than $1,000.
The
accompanying notes are an integral part of the financial
statements.
F-6
XTL
BIOPHARMACEUTICALS LTD.
(A
Development Stage Company)
CONSOLIDATED
STATEMENTS OF CHANGES IN SHAREHOLDERS' EQUITY (continued)
(in
thousands of U.S. dollars, except share amounts)
|
Deficit
|
||||||||||
|
Accumulated
|
accumulated
|
|||||||||
|
other
|
during
the
|
|||||||||
|
comprehensive
|
development
|
|||||||||
|
income
(loss)
|
stage
|
Total
|
||||||||
|
CHANGES
DURING THE PERIOD
|
||||||||||
|
FROM
MARCH 9, 1993 (DATE OF
|
||||||||||
|
INCORPORATION)
TO
DECEMBER
31, 2002 :
|
||||||||||
|
Comprehensive
loss:
|
||||||||||
|
Loss
for the period
|
—
|
(55,015
|
)
|
(55,015
|
)
|
|||||
|
Net
unrealized loss
|
(48
|
)
|
—
|
(48
|
)
|
|||||
|
Comprehensive
loss
|
(48
|
)
|
(55,015
|
)
|
(55,063
|
)
|
||||
|
Employee
stock options expenses
|
—
|
—
|
377
|
|||||||
|
Non-employee
stock option expenses
|
—
|
—
|
106
|
|||||||
|
Exercise
of share warrants in 2000
|
—
|
—
|
347
|
|||||||
|
Exercise
of share warrants in 2001
|
—
|
—
|
75
|
|||||||
|
Exercise
of employee stock
options
in 1999
|
—
|
—
|
**
|
|||||||
|
Exercise
of employee stock
options
in 2000
|
—
|
—
|
1
|
|||||||
|
Exercise
of employee stock
options
in 2001
|
—
|
26
|
||||||||
|
Exercise
of employee stock
options
in 2002
|
—
|
20
|
||||||||
|
Issuance
of share capital in 1993 (net
of
$912 - issuance expenses)
|
—
|
—
|
5,590
|
|||||||
|
Issuance
of share capital in 1994 (net
of
$22 - issuance expenses)
|
—
|
—
|
2,108
|
|||||||
|
Issuance
of share capital in 1996 (net
of
$646 - issuance expenses)
|
—
|
—
|
5,363
|
|||||||
|
Issuance
of share capital in 1998 (net
of
$1,650 - issuance expenses)
|
—
|
—
|
12,175
|
|||||||
|
Issuance
of share capital in 1999 (net
of
$49 - issuance expenses)
|
—
|
—
|
1,201
|
|||||||
|
Issuance
of share capital in 2000
|
—
|
—
|
16,702
|
|||||||
|
Bonus
shares
|
—
|
—
|
—
|
|||||||
|
Conversion
of preferred shares into
|
||||||||||
|
ordinary
shares
|
—
|
—
|
—
|
|||||||
|
Receipts
in respect of share warrants
|
||||||||||
|
(expired
in 1999)
|
—
|
—
|
89
|
|||||||
|
Initial
public offering (“IPO”) of the
|
||||||||||
|
Company’s
shares under a prospectus
|
||||||||||
|
dated
September 20, 2000 (net of
|
||||||||||
|
$ 5,199
-issuance expenses)
|
—
|
—
|
45,713
|
|||||||
|
BALANCE
AT DECEMBER 31, 2002
|
(48
|
)
|
(55,015
|
)
|
34,830
|
|||||
The
accompanying notes are an integral part of the financial
statements.
F-7
XTL
BIOPHARMACEUTICALS LTD.
(A
Development Stage Company)
CONSOLIDATED
STATEMENTS OF CHANGES IN SHAREHOLDERS’ EQUITY (continued)
(in
thousands of U.S. dollars, except share amounts)
|
Ordinary
shares
|
Additional
|
|||||||||
|
Number
of
|
paid
in
|
|||||||||
|
shares
|
Amount
|
capital
|
||||||||
|
BALANCE
AT DECEMBER 31, 2002 -
brought
forward
|
111,165,364
|
590
|
89,303
|
|||||||
|
CHANGES
DURING 2003:
|
||||||||||
|
Comprehensive
loss:
|
||||||||||
|
Loss
for the period
|
—
|
—
|
—
|
|||||||
|
Net
unrealized gain
|
—
|
—
|
—
|
|||||||
|
Comprehensive
loss
|
—
|
—
|
—
|
|||||||
|
Exercise
of stock options
|
854,100
|
4
|
—
|
|||||||
|
BALANCE
AT DECEMBER 31, 2003
|
112,019,464
|
594
|
89,303
|
|||||||
|
CHANGES
DURING 2004:
|
||||||||||
|
Comprehensive
loss:
|
||||||||||
|
Net
loss
|
—
|
—
|
—
|
|||||||
|
Net
unrealized loss
|
—
|
—
|
—
|
|||||||
|
Comprehensive
loss
|
—
|
—
|
—
|
|||||||
|
Non-employee
stock option compensation expenses
|
—
|
—
|
32
|
|||||||
|
Exercise
of stock options
|
50,000
|
**
|
19
|
|||||||
|
Issuance
of shares, net of $2,426
share
issuance expenses
|
56,009,732
|
247
|
15,183
|
|||||||
|
BALANCE
AT DECEMBER 31, 2004
|
168,079,196
|
841
|
104,537
|
|||||||
|
CHANGES
DURING 2005:
|
||||||||||
|
Comprehensive
loss - loss for the period
|
— | — | — | |||||||
|
Non-employee
stock option compensation expenses
|
—
|
—
|
45
|
|||||||
|
Employee
stock option compensation expenses
|
—
|
—
|
2,718
|
|||||||
|
Exercise
of stock options
|
3,786,825
|
17
|
1,494
|
|||||||
|
Issuance
of ordinary shares in respect of license
|
||||||||||
|
and
purchases of assets (Note 3)
|
1,314,420
|
6
|
1,385
|
|||||||
|
BALANCE
AT DECEMBER 31, 2005
|
173,180,441
|
864
|
110,179
|
|||||||
** Represents
an amount less than $ 1,000.
The
accompanying notes are an integral part of the financial
statements.
F-8
XTL
BIOPHARMACEUTICALS LTD.
(A
Development Stage Company)
CONSOLIDATED
STATEMENTS OF CHANGES IN SHAREHOLDERS’ EQUITY (continued)
(in
thousands of U.S. dollars, except share amounts)
|
Deficit
|
||||||||||
|
Accumulated
|
accumulated
|
|||||||||
|
other
|
during
the
|
|||||||||
|
comprehensive
|
development
|
|||||||||
|
income
(loss)
|
stage
|
Total
|
||||||||
|
BALANCE
AT DECEMBER 31, 2002 -
|
||||||||||
|
brought
forward
|
(48
|
)
|
(55,015
|
)
|
34,830
|
|||||
|
CHANGES
DURING 2003:
|
||||||||||
|
Comprehensive
loss:
|
||||||||||
|
Loss
for the period
|
—
|
(14,288
|
)
|
(14,288
|
)
|
|||||
|
Net
unrealized gain
|
62
|
—
|
62
|
|||||||
|
Comprehensive
loss
|
62
|
(14,288
|
)
|
(14,226
|
)
|
|||||
|
Exercise
of stock options
|
—
|
—
|
4
|
|||||||
|
BALANCE
AT DECEMBER 31, 2003
|
14
|
(69,303
|
)
|
20,608
|
||||||
|
CHANGES
DURING 2004:
|
||||||||||
|
Comprehensive
loss:
|
||||||||||
|
Loss
for the period
|
—
|
(16,473
|
)
|
(16,473
|
)
|
|||||
|
Net
unrealized loss
|
(14
|
)
|
—
|
(14
|
)
|
|||||
|
Comprehensive
loss
|
(14
|
)
|
(16,473
|
)
|
(16,487
|
)
|
||||
|
Non-employee
stock option expenses
|
—
|
—
|
32
|
|||||||
|
Exercise
of stock options
|
—
|
—
|
19
|
|||||||
|
Issuance
of shares, net of $2,426
|
||||||||||
|
share
issuance expenses
|
—
|
—
|
15,430
|
|||||||
|
BALANCE
AT DECEMBER 31, 2004
|
—
|
(85,776
|
)
|
19,602
|
||||||
|
CHANGES
DURING 2005:
|
||||||||||
|
Comprehensive
loss - loss for the period
|
—
|
(14,015
|
)
|
(14,015
|
)
|
|||||
|
Non-employee
stock option compensation expenses
|
—
|
—
|
45
|
|||||||
|
Employee
stock option compensation expenses
|
—
|
—
|
2,718
|
|||||||
|
Exercise
of stock options
|
—
|
—
|
1,511
|
|||||||
|
Issuance
of ordinary shares in respect of license
|
||||||||||
|
and
purchases of assets (Note 3)
|
—
|
—
|
1,391
|
|||||||
|
BALANCE
AT DECEMBER 31, 2005
|
—
|
(99,791
|
)
|
11,252
|
||||||
The
accompanying notes are an integral part of the financial
statements.
F-9
XTL
BIOPHARMACEUTICALS LTD.
(A
Development Stage Company)
(in
thousands of U.S. dollars)
|
Period
from
|
|||||||||||||
|
March
9, 1993 (a)
|
|||||||||||||
|
Year
ended December 31
|
to
December 31,
|
||||||||||||
|
2005
|
2004
|
2003
|
2005
|
||||||||||
|
CASH
FLOWS FROM OPERATING ACTIVITIES:
|
|||||||||||||
|
Loss
for the period
|
(14,015
|
)
|
(16,473
|
)
|
(14,288
|
)
|
(99,791
|
)
|
|||||
|
Adjustments
to reconcile loss to net cash used in operating
activities:
|
|||||||||||||
|
Depreciation
and amortization
|
242
|
319
|
440
|
2,829
|
|||||||||
|
Linkage
difference on restricted long-term deposits
|
3
|
—
|
—
|
3
|
|||||||||
|
Acquisition
of in process research and development
|
1,783
|
—
|
—
|
1,783
|
|||||||||
|
Loss
on disposal of property and equipment
|
6
|
1
|
2
|
18
|
|||||||||
|
Increase
(decrease) in liability in respect of employee severance
obligations
|
(159
|
)
|
30
|
129
|
1,228
|
||||||||
|
Impairment
charges
|
26
|
—
|
354
|
380
|
|||||||||
|
Loss
(gain) from sales of available for sale securities
|
—
|
13
|
(27
|
)
|
(410
|
)
|
|||||||
|
Stock
based compensation expenses (employee and non-employee)
|
2,763
|
32
|
—
|
3,278
|
|||||||||
|
Loss
(gain) on amounts funded in respect of employee severance pay
funds
|
(6
|
)
|
(4
|
)
|
5
|
(91
|
)
|
||||||
|
Changes
in operating assets and liabilities:
|
|||||||||||||
|
Decrease
(increase) in accounts receivable - trade
|
543
|
(543
|
)
|
—
|
—
|
||||||||
|
Decrease
(increase) in accounts receivable - other
|
(125
|
)
|
400
|
(440
|
)
|
(431
|
)
|
||||||
|
Increase
(decrease) in accounts payable and accruals
|
(1,127
|
)
|
133
|
499
|
2,007
|
||||||||
|
Increase
(decrease) in deferred gain
|
(400
|
)
|
1,597
|
—
|
1,197
|
||||||||
|
Net
cash used in operating activities
|
(10,466
|
)
|
(14,495
|
)
|
(13,326
|
)
|
(88,000
|
)
|
|||||
|
CASH
FLOWS FROM INVESTING ACTIVITIES:
|
|||||||||||||
|
Decrease
in short-term deposits
|
10,136
|
7,193
|
14,724
|
—
|
|||||||||
|
Restricted
long-term deposits, net
|
—
|
46
|
(20
|
)
|
(113
|
)
|
|||||||
|
Investment
in available for sale securities
|
—
|
—
|
(71
|
)
|
(3,363
|
)
|
|||||||
|
Proceeds
from sales of available for sale securities
|
—
|
722
|
1,048
|
3,773
|
|||||||||
|
Employee
severance
pay funds
|
(50
|
)
|
(136
|
)
|
(112
|
)
|
(891
|
)
|
|||||
|
Purchase
of property and equipment
|
(38
|
)
|
(180
|
)
|
(81
|
)
|
(4,021
|
)
|
|||||
|
Proceeds
from disposals of property and equipment
|
27
|
5
|
2
|
149
|
|||||||||
|
Acquisition
in respect of license and purchase of assets
|
(548
|
)
|
—
|
—
|
(548
|
)
|
|||||||
|
Net
cash provided by (used in) investing activities
|
9,527
|
7,650
|
15,490
|
(5,014
|
)
|
||||||||
F-10
XTL
BIOPHARMACEUTICALS LTD.
(A
Development Stage Company)
CONSOLIDATED
STATEMENTS OF CASH FLOWS (continued)
(in
thousands of U.S dollars)
|
Period
from
|
|||||||||||||
|
March
9, 1993 (a)
|
|||||||||||||
|
Year
ended December 31
|
to
December 31,
|
||||||||||||
|
2005
|
2004
|
2003
|
2005
|
||||||||||
|
CASH
FLOWS FROM FINANCING ACTIVITIES:
|
|||||||||||||
|
Issuance
of share capital - net of share issuance expenses
|
—
|
15,430
|
—
|
104,371
|
|||||||||
|
Exercise
of share warrants and stock options
|
1,511
|
19
|
4
|
2,003
|
|||||||||
|
Proceeds
from long-term debt
|
—
|
—
|
—
|
399
|
|||||||||
|
Proceeds
from short-term debt
|
—
|
—
|
—
|
50
|
|||||||||
|
Repayment
of long-term debt
|
—
|
—
|
—
|
(399
|
)
|
||||||||
|
Repayment
of short-term debt
|
—
|
—
|
—
|
(50
|
)
|
||||||||
|
Net
cash provided by financing activities
|
1,511
|
15,449
|
4
|
106,374
|
|||||||||
|
NET
INCREASE (DECREASE) IN CASH AND
|
|||||||||||||
|
CASH
EQUIVALENTS
|
572
|
8,604
|
2,168
|
13,360
|
|||||||||
|
BALANCE
OF CASH AND CASH EQUIVALENTS AT BEGINNING
OF PERIOD
|
12,788
|
4,184
|
2,016
|
—
|
|||||||||
|
BALANCE
OF CASH AND CASH EQUIVALENTS AT END OF
PERIOD
|
13,360
|
12,788
|
4,184
|
13,360
|
|||||||||
|
Supplementary
information on investing and financing
activities not involving cash flows:
|
|||||||||||||
|
Issuance
of ordinary shares in respect of license,
and purchase of assets
|
1,391
|
—
|
—
|
1,391
|
|||||||||
|
Conversion
of convertible subordinated debenture into shares
|
—
|
—
|
—
|
1,700
|
|||||||||
|
Supplemental
disclosures of cash flow information:
|
|||||||||||||
|
Income
taxes paid (mainly - tax advance in respect of excess
expenses)
|
49
|
107
|
161
|
321
|
|||||||||
|
Interest
paid
|
—
|
—
|
—
|
350
|
|||||||||
|
(a) Incorporation
date, see note 1a.
|
|||||||||||||
The
accompanying notes are an integral part of the financial
statements.
F-11
XTL
BIOPHARMACEUTICALS LTD.
(A
Development Stage Company)
NOTE
1 - SIGNIFICANT ACCOUNTING POLICIES:
a. General:
|
1)
|
XTL
Biopharmaceuticals Ltd. (“the Company”) was incorporated under the Israel
Companies Ordinance on March 9, 1993. The Company is a development
stage
company in accordance with Financial Accounting Standard (“FAS”) 7
“Accounting and Reporting by Development Stage Enterprises.”
The
Company is a biopharmaceutical company engaged in the acquisition,
development and commercialization of pharmaceutical products
for the
treatment of infectious diseases, particularly the prevention
and
treatment of hepatitis B and C.
The
Company licensed its product candidate HepeX-B to Cubist Pharmaceuticals,
Inc. (hereinafter “Cubist”) during 2004, see Notes 1k and 2 as to details
of the agreement.
During
September 2005, the Company licensed perpetually from VivoQuest
Inc.
(“VivoQuest”), a US privately-held company which is a development stage
enterprise, exclusive worldwide rights to VivoQuest’s intellectual
property and technology, covering a proprietary compound library,
including VivoQuest’s lead hepatitis C compounds. In addition, the Company
also acquired from VivoQuest certain assets, see Note 3.
The
Company has a wholly-owned subsidiary in the United States, XTL
Biopharmaceuticals Inc. (“Subsidiary”), which was incorporated in 1999
under the law of the State of Delaware. The Subsidiary is primarily
engaged in development activities and business
development.
|
|
2)
|
The
consolidated financial statements of the Company are presented on
a going
concern basis, which contemplates the realization of assets and
satisfaction of liabilities in the normal course of business. The
Company
has experienced a significant loss from operations. For the year
ended
December 31, 2005, the Company incurred a net loss of $14 million
and had
an accumulated deficit of $100 million. These matters raise substantial
doubt about the Company’s ability to continue as a going concern.
The
Company’s ability to continue as a going concern will depend upon its
ability to raise additional capital in the short term. The Company
is
actively pursuing raising additional capital to fund its operations
although there is no assurance that such capital will be available
to the
Company. Failure to secure additional capital or to expand its revenue
base would result in the Company depleting its available funds and
not
being able to pay its obligations when they become due. The accompanying
consolidated financial statements do not include any adjustments
to
reflect the possible future effects on the recoverability and
classification of assets or the amounts and
classification of liabilities that may result from the possible inability
of the Company to continue as a going
concern.
|
|
3)
|
The
consolidated financial statements are prepared in accordance with
generally accepted accounting principles in the United States (“US
GAAP”).
|
|
4)
|
The
preparation of the financial statements, in conformity with US GAAP,
requires management to make estimates and assumptions that affect
the
reported amounts of assets and liabilities and the disclosure of
contingent assets and liabilities, at the date of the financial
statements, and the reported expenses during the reporting periods.
Actual
results may vary from these
estimates.
|
F-12
XTL
BIOPHARMACEUTICALS LTD.
(A
Development Stage Company)
NOTES
TO
THE CONSOLIDATED FINANCIAL STATEMENTS (continued)
NOTE
1 - SIGNIFICANT ACCOUNTING POLICIES (continued):
b. Functional
currency
The
currency of the primary economic environment in which the operations of the
Company are conducted is the U.S. dollar ("$" or "dollar").
Most
of
the Company's expenses and revenues are incurred in dollars. A significant
part
of the Company's capital expenditures and most of its external financing is
in
dollars. The Company holds most of its cash, cash equivalents and bank deposits
in dollars.
Thus,
the
functional currency of the Company is dollar.
Since
the
dollar is the primary currency in the economic environment in which the Company
operates, monetary accounts maintained in currencies other than the dollar
(principally cash and liabilities) are remeasured using the representative
foreign exchange rate at the balance sheet date. Operational accounts and
nonmonetary balance sheet accounts are measured and recorded at the rate in
effect at the date of the transaction. The effects of foreign currency
remeasurement are reported in current operations (as “financial income - net”)
and have not been material to date.
c. Principles
of consolidation
The
consolidated financial statements include the accounts of the Company and its
wholly-owned subsidiary. All intercompany transactions and balances were
eliminated in consolidation.
d. Impairment
of long-lived assets
Pursuant
to FAS 144 “Accounting for the Impairment or Disposal of Long-Lived Assets”
(“FAS 144”), long-lived assets, including certain intangible assets, to be
held and used by an entity, are reviewed for impairment whenever events or
changes in circumstances indicate that the carrying amount of the assets may
not
be recoverable. Under FAS 144, if the sum of the expected future cash flows
(undiscounted and without interest charges) of the long-lived assets held and
used is less than the carrying amount of such assets, an impairment loss would
be recognized, and the assets are written down to their estimated fair values.
Assets “held for sale” are reported at the lower of their carrying amount or
fair value less estimated costs to sell. As to the impairment charges recognized
by the Company, see Note 4b.
e. Cash
equivalents
Highly
liquid investments, which include short-term bank deposits (up to three months
from date of deposit), that are not restricted as to withdrawal or use, are
considered by the Company to be cash equivalents.
F-13
XTL
BIOPHARMACEUTICALS LTD.
(A
Development Stage Company)
NOTES
TO
THE CONSOLIDATED FINANCIAL STATEMENTS (continued)
NOTE
1 - SIGNIFICANT ACCOUNTING POLICIES (continued):
f. Marketable
securities
Pursuant
to FAS No. 115, "Accounting for Certain Investments in Debt and Equity
Securities," the Company's investment in debt securities (mainly debentures)
have been designated as available-for-sale. Available-for-sale securities are
carried at fair value, which is determined based upon the quoted market prices
of the securities, with unrealized gains and losses reported in accumulated
other comprehensive income, a component of shareholders' equity. Realized gains
and losses and declines in value judged to be other than temporary on
available-for-sale securities are included in “financial income, net.” The
Company viewed its available-for-sale portfolio as available for use in its
current operations. Interest, premium and discount amortization, and dividends
on securities classified as available-for-sale are included in “financial
income, net”. As of December 31, 2005 and 2004, the Company did not have any
available for sale securities.
g. Property
and equipment
These
assets are carried at cost less depreciation, amortization and impairment
charges. Depreciation is computed using the straight-line method over the
estimated useful life of the assets.
Annual
rates of depreciation are as follows:
|
%
|
|
|
Laboratory
equipment
|
10-20
|
|
(mainly
15)
|
|
|
Computers
|
33
|
|
Furniture
and office equipment
|
6-15
|
Leasehold
improvements are amortized by the straight-line method over the term of the
lease, which is shorter than the estimated useful life of the
improvements.
h.
Intangible
assets
Intangible
assets consist of the assembled workforce in respect of the license and purchase
of certain assets from VivoQuest Inc. (see Note 3). The intangible assets are
amortized using the straight- line method over its estimated useful life of
3
years.
i. Deferred
income taxes
Deferred
taxes are determined utilizing the asset and liability method based on the
estimated future tax effects of differences between the financial accounting
and
tax basis of assets and liabilities under the applicable tax laws. Deferred
tax
balances are computed using the tax rates expected to be in effect when these
differences reversed. Valuation allowances are provided if, based upon the
weight of available evidence, it is more likely than not that some or all of
the
deferred tax assets will not be realized.
Paragraph
9(f) of FAS 109, “Accounting for Income Taxes,” prohibits the recognition
of deferred tax liabilities or assets that arise from differences between the
financial reporting and tax basis of assets and liabilities that are measured
from the local currency into dollars using historical exchange rates, and that
result from changes in exchange rates or indexing for tax purposes.
Consequently, the abovementioned differences were not reflected in the
computation of deferred tax assets and liabilities.
F-14
XTL
BIOPHARMACEUTICALS LTD.
(A
Development Stage Company)
NOTES
TO
THE CONSOLIDATED FINANCIAL STATEMENTS (continued)
NOTE
1 - SIGNIFICANT ACCOUNTING POLICIES (continued):
j. Research
and development costs and participations
Research
and development costs are expensed as they are incurred and consist primarily
of
salaries and related personnel costs, fees paid to consultants and other
third-parties for clinical and laboratory development, facilities-related and
other expenses relating to the design, development, testing, and enhancement
of
product candidates.
Participations
from government (and from others) for development of approved projects are
recognized as a reduction of expense as the related costs are incurred (see
Note
7).
In
connection with purchase of assets, amounts assigned to intangible assets to
be
used in a particular research and development project that have not reached
technological feasibility and have no alternative future use are charged to
in-
process research and development costs at the purchase date.
k. Revenue
recognition
The
Company recognizes the revenue from the licensing agreement with Cubist (see
Note 2) under the provisions of the EITF 00-21 “Revenue Arrangements with
Multiple Deliverables” and SAB 104 “Revenue Recognition.” Under those
pronouncements, companies are required to allocate revenues from
multiple-element arrangements to the different elements based on sufficient
objective and reliable evidence of fair value. Since the Company does not have
the ability to determine the fair value of each unit of accounting, the
agreement was accounted for as one unit of accounting, after failing the
separation criteria, and the Company recognizes each payment on the
abovementioned agreement ratably over the expected life of the
arrangement.
In
addition, through 2005, Cubist had requested that the Company provide
development services to be reimbursed by Cubist. As required by EITF 01-14
“Income Statement Characterization of Reimbursements Received for
"Out-of-Pocket" Expenses Incurred,” amounts paid by the Company, as a principal,
are included in the cost of revenues as reimbursable out-of-pocket expenses,
and
the reimbursements the Company receives as a principal are reported as
reimbursed out-of-pocket revenues.
l. Business
development costs
Costs
associated with business development are comprised of costs related to
partnering activities for the Company’s drug programs and for seeking new
development collaborations. Business development expenses are expensed as
incurred.
F-15
XTL
BIOPHARMACEUTICALS LTD.
(A
Development Stage Company)
NOTES
TO
THE CONSOLIDATED FINANCIAL STATEMENTS (continued)
NOTE
1 - SIGNIFICANT ACCOUNTING POLICIES (continued):
m. Loss
per share (“LPS”)
Basic
and
diluted losses per share are presented in accordance with FAS No. 128 “Earnings
per share” (“FAS 128”), for all the years presented. Outstanding share options,
and warrants have been excluded from the calculation of the diluted loss per
share because all such securities are antidilutive for all the years presented.
The total weighted average number of ordinary shares related to outstanding
options and warrants excluded from the calculations of diluted loss per share
were 20,807,875, 18,187,062 and 17,721,724 for the years ended December 31,
2005, 2004 and 2003, respectively.
n. Comprehensive
loss
Comprehensive
loss, included in shareholders' equity, consists of the loss for each period
presented, and for the years ended December 31, 2004 and 2003, also includes
the
net unrealized gains or losses on available for sale marketable
securities.
o. Stock-
based compensation
Prior
to
January 1, 2005, the Company accounted for employee stock-based compensation
under the intrinsic value model in accordance with Accounting Principles Board
Opinion No. 25 - “Accounting for Stock Issued to Employees” (“APB 25”) and
related interpretations. Under APB 25, compensation expense is based on the
difference, if any, on the date of the grant, between the fair value of the
Company’s ordinary shares and the exercise price. When the number of the
underlying shares or the exercise price is not known at the grant date, the
Company updated, at each period, the compensation expenses until such data
becomes known. In addition, in accordance with FAS 123 No. “Accounting for
Stock-Based Compensation” (“FAS 123”), which was issued by the Financial
Accounting Standards Board ("FASB"), the Company disclosed pro forma data
assuming it had accounted for employee share option grants using the fair
value-based method defined in FAS 123.
In
December 2004, the FASB issued the revised FAS No. 123R “Share - Based Payment”
(“FAS 123R”), which addresses the accounting for share-based payment
transactions in which a company obtains employee services in exchange for (a)
equity instruments of a company or (b) liabilities that are based on the fair
value of a company’s equity instruments or that may be settled by the issuance
of such equity instruments. In March 2005, the SEC issued Staff Accounting
Bulletin No. 107 (“SAB 107”) regarding the SEC's interpretation of FAS
123R.
FAS
123R
eliminates the ability to account for employee share-based payment transactions
using APB 25, and requires instead that such transactions be accounted for
using
the grant-date fair value based method. FAS 123R is effective as of the annual
reporting period that begins after June 15, 2005. Early adoption of FAS
123R is encouraged. FAS 123R applies to all awards granted or modified after
the
effective date of the standard. In addition, compensation cost for the unvested
portion of previously granted awards that remain outstanding on the effective
date shall be recognized on or after the effective date, as the related services
are rendered, based on the awards’ grant-date fair value as previously
calculated for the pro-forma disclosure under FAS 123.
The
Company implemented early adoption of FAS 123R, as of January 1, 2005, using
the
modified prospective application transition method, as permitted by FAS 123R.
Under such transition method, the Company’s financial statements for periods
prior to the effective date of FAS 123R (January 1, 2005) have not been
restated. As a result of the early adoption, the Company reduced the deferred
share-based compensation against the additional paid in capital.
F-16
XTL
BIOPHARMACEUTICALS LTD.
(A
Development Stage Company)
NOTES
TO
THE CONSOLIDATED FINANCIAL STATEMENTS (continued)
NOTE
1 - SIGNIFICANT ACCOUNTING POLICIES (continued):
The
fair
value of stock
options
granted
with service conditions, was determined using the Black-Scholes valuation model,
which is consistent with the Company’s valuation techniques previously utilized
for options in footnote disclosures required under FAS 123, as amended by FAS
No. 148, “Accounting for Stock-Based Compensation - Transition and
Disclosure.” Such value is recognized as an expense over the service period, net
of estimated forfeitures, using the straight-line method under FAS 123R. The
fair value of stock options granted with market conditions, was determined
using
a lattice model that incorporated a Monte Carlo Simulation method. Such value
is
recognized as an expense using the graded method under FAS123R.
The
estimation of stock awards that will ultimately vest requires significant
judgment, and to the extent actual results or updated estimates differ from
the
Company’s current estimates, such amounts will be recorded as a cumulative
adjustment in the period those estimates are revised. The Company considers
many
factors when estimating expected forfeitures, including types of awards,
employee class, and historical experience. Actual results, and future changes
in
estimates, may differ substantially from the Company’s current estimates.
Both
the
Black-Scholes model and a lattice model incorporating the Monte Carlo simulation
method, take into account a number of valuation parameters, see also Note
6.
The
application of FAS 123R had the following effect on reported amounts, for the
year ended December 31, 2005, relative to amounts that would have been reported
using the intrinsic value method under previous accounting ($ in thousands,
except per share amounts):
|
Using
previous
accounting
|
Impact
of the adoption of
FAS
123R
|
As
reported
|
|
| Loss for the year |
12,130
|
1,885
|
14,015
|
| Basic and diluted loss per ordinary share |
(0.07)
|
(0.08)
|
F-17
XTL
BIOPHARMACEUTICALS LTD.
(A
Development Stage Company)
NOTES
TO
THE CONSOLIDATED FINANCIAL STATEMENTS (continued)
NOTE
1 - SIGNIFICANT ACCOUNTING POLICIES (continued):
The
following table illustrates the effect on loss and loss per share assuming
the
Company had applied the fair value recognition provisions of FAS 123 to its
stock-based employee compensation, for years presented prior to the adoption
of
FAS 123R:
|
Period
from
|
||||||||||
|
March
9, 1993*
|
||||||||||
|
Year
ended December 31
|
to
December 31,
|
|||||||||
|
2004
|
2003
|
2004
|
||||||||
|
($
in thousands except per share amounts)
|
||||||||||
|
Loss
for the period, as reported
|
16,473
|
14,288
|
85,776
|
|||||||
|
Deduct:
stock- based employee
|
||||||||||
|
compensation
expense,
|
||||||||||
|
included
in reported loss
|
—
|
—
|
(483
|
)
|
||||||
|
Add:
stock-based employee
|
||||||||||
|
compensation
expense
|
||||||||||
|
determined
under fair value
|
||||||||||
|
method
for all awards
|
239
|
821
|
6,355
|
|||||||
|
Loss
- pro-forma
|
16,712
|
15,109
|
91,648
|
|||||||
|
Basic
and diluted loss per share:
|
||||||||||
|
As
reported
|
0.12
|
0.13
|
||||||||
|
Pro-forma
|
0.12
|
0.14
|
||||||||
*
Incorporation date, see note 1a.
The
Company accounts for equity instruments issued to third party service providers
(non - employees) in accordance with the fair value method prescribed by FAS123,
and as of January 1, 2005, by FAS 123R, and the provisions Emerging Issues
Task
Force Issue No. 96-18, “Accounting for Equity Instruments That Are Issued to
Other Than Employees for Acquiring, or in Conjunction with Selling Goods or
Services” (“EITF 96-18”). See note 6 b (3).
F-18
XTL
BIOPHARMACEUTICALS LTD.
(A
Development Stage Company)
NOTES
TO
THE CONSOLIDATED FINANCIAL STATEMENTS (continued)
NOTE
1 - SIGNIFICANT ACCOUNTING POLICIES (continued):
p. Recently
issued accounting pronouncements in the United States:
FAS
No.153 “Exchanges of Nonmonetary Assets - An Amendment of APB Opinion No.
29”
In
December 2004, the FASB issued FAS No. 153 “Exchanges of Nonmonetary Assets - An
Amendment of APB Opinion No. 29” (‘FAS 153”). FAS 153 amends APB Opinion
No. 29 “Accounting for Nonmonetary Transactions” (“APB 29”). The amendments made
by FAS 153 are based on the principle that exchanges of nonmonetary assets
should be measured based on the fair value of the assets exchanged. Further,
the
amendments eliminate the exception for nonmonetary exchanges of similar
productive assets and replace it with a general exception for exchanges of
nonmonetary assets that do not have commercial substance. The provisions in
FAS
153 are effective for nonmonetary asset exchanges occurring in fiscal periods
beginning after December 15, 2005 (January 1, 2006 for the Company). Early
application of the FAS 153 is permitted. The provisions of this Statement shall
be applied prospectively. The Company does not expect the adoption of FAS
153 to have a material effect on its financial statements or its results of
operations.
FAS
No.
154 “Accounting Changes and Error Corrections - a replacement of APB Opinion No.
20 and FASB Statement No. 3”
In
May
2005, the FASB issued FAS No. 154 "Accounting Changes and Error Corrections
- a
replacement of APB Opinion No. 20 (“APB 20”) and FASB Statement No. 3". FAS 154
generally requires retrospective application to prior periods' financial
statements of changes in accounting principle. Previously, APB 20 required
that
most voluntary changes in accounting principle were recognized by including
the
cumulative effect of changing to the new accounting principle in the net income
of the period of the change. FAS 154 applies to all voluntary changes in
accounting principle. It also applies to changes required by an accounting
pronouncement in the unusual instance that the pronouncement does not include
specific transition provisions. When a pronouncement includes specific
transition provisions, those provisions should be followed. FAS 154 shall be
effective for accounting changes and corrections of errors made in fiscal years
beginning after December15, 2005 (January 1, 2006 for the Company). The Company
does not expect the adoption of this statement will have a material impact
on
its financial statements or its results of operations.
q. Reclassifications
Certain
comparative figures have been reclassified to conform to the current year
presentation.
F-19
XTL
BIOPHARMACEUTICALS LTD.
(A
Development Stage Company)
NOTES
TO
THE CONSOLIDATED FINANCIAL STATEMENTS (continued)
NOTE
2 - LICENSE AGREEMENT WITH CUBIST
The
Company entered into a licensing agreement with Cubist in June 2004, under
which
the Company granted to Cubist an exclusive, worldwide license (with the right
to
sub-license) to commercialize HepeX-B and any other product containing an hMAb,
or humanized monoclonal antibody, or fragment directed at the hepatitis B virus
owned or controlled by the Company. See Note 1k for the revenue recognition
treatment.
In
August
2005, the Company amended its licensing agreement with Cubist. Under the terms
of the agreement, as amended, Cubist paid the Company an initial up front
nonrefundable payment of $1 million upon the signing of the agreement, and
a
payment of $1 million (out of which $454,000 and $185,000 was recorded as
revenue in the years ended December 31, 2005 and 2004, respectively) as
collaboration support paid in 2004 (instead of a total of $2 million to be
paid
in installments through 2005, as per the original agreement). Furthermore under
the terms of the agreement, as amended, Cubist shall make a payment in the
amount of $3 million upon achievement of certain regulatory milestones until
the
end of 2007 or an amount of $2 million upon achievement of the same certain
regulatory milestones until the end of 2008. Under this agreement, as amended,
the Company was responsible for certain clinical and product development
activities of HepeX-B through August 2005, at the expense of Cubist. The Company
has transferred full responsibility for completing the development of HepeX-B
to
Cubist. Cubist will be responsible for completing the development and for
registration and commercialization of the product worldwide.
F-20
XTL
BIOPHARMACEUTICALS LTD.
(A
Development Stage Company)
NOTES
TO
THE CONSOLIDATED FINANCIAL STATEMENTS (continued)
NOTE
2 - LICENSE AGREEMENT WITH CUBIST
(continued):
The
Company accounts for the payments resulting from the agreement, as follows
(i)
the $1 million up-front fee and the collaboration support payments are recorded
as deferred revenue upon receipt, and amortized through 2008 or date regulatory
approval are reached, if earlier, and (ii) the milestone contingent payments
will be recorded as revenue when regulatory approval milestones are
obtained.
Under
the
agreement, the Company is entitled to receive royalties from net sales by
Cubist, if any, generally ranging from 10% to 17%, depending on levels of net
sales achieved by Cubist, subject to certain deductions based on patent
protection of HepeX-B in that territory, total cost of HepeX-B development,
third party license payments and indemnification obligations.
The
agreement expires on the later of the last valid patent claim covering Hepex-B
to expire, or 10 years after the first commercial sale of HepeX-B on a
country-by-country basis.
Under
a
research and license agreement with Yeda (see Note 7a(1)), the Company paid
during 2004, $250,000 with respect to the $1 million up front fee received
in
June 2004, out of which $54,000 and $32,000 was recorded as cost of revenues
in
2005 and 2004, respectively.
The
balance of the deferred gain, related to the revenue from Cubist, as of December
31, 2004 and 2005, was presented in the balance sheet, net of the above
mentioned payment, as follows:
|
December
31,
|
|||||||
|
2005
|
2004
|
||||||
|
($
in thousands)
|
|||||||
|
Deferred
revenue
|
1,361
|
1,815
|
|||||
|
Less
- Deferred expenses related to Yeda
|
164
|
218
|
|||||
|
Deferred
gain
|
1,197
|
1,597
|
|||||
For
the
commitment to the Government of Israel, related to the transfer of manufacturing
rights of the Company’s HepeX-B product candidate, under the terms of the
agreement with Cubist, see Note 7a(2).
F-21
XTL
BIOPHARMACEUTICALS LTD.
(A
Development Stage Company)
NOTES
TO
THE CONSOLIDATED FINANCIAL STATEMENTS (continued)
NOTE
3 - LICENSE AND ASSET PURCHASE AGREEMENT WITH VIVOQUEST
During
September 2005, the Company licensed perpetually from VivoQuest Inc.
(“VivoQuest”), a US privately-held company, which is a development stage
enterprise, exclusive worldwide rights to VivoQuest’s intellectual property and
technology, covering a proprietary compound library, including VivoQuest’s lead
hepatitis C compounds. In addition, the Company acquired from VivoQuest certain
assets, including VivoQuest’s laboratory equipment, assumed VivoQuest’s lease of
its laboratory space and certain research and development employees. The Company
executed this transaction in order to broaden its pipeline and strengthen its
franchise in infectious diseases.
In
connection with the VivoQuest transaction (the “Transaction”):
| (1) |
the
Company issued the fair value equivalent of $1,391,000 of its ordinary
shares for a total of 1,314,420 ordinary shares (calculated based
upon the
average of the closing prices per share for the period commencing
two days
before, and ending two days after the closing of the transaction),
made
cash payments of approximately $400,000 to cover VivoQuest’s operating
expenses prior to the closing of the Transaction, and incurred $148,000
in
direct expenses associated with the
Transaction;
|
| (2) |
the
Company agreed to make additional contingent milestone payments triggered
by certain regulatory and sales targets, totaling up to $34.6 million,
$25.0 million of which will be due upon or following regulatory approval
or actual product sales, and are payable in cash or ordinary shares
at the
Company’s election. No contingent consideration has been paid pursuant to
the license agreement as of the balance sheet date, because none
of the
milestones have been achieved. The contingent consideration will
be
recorded as part of the acquisition costs in the future; and
|
| (3) |
the
Company agreed to make royalty payments on future product
sales.
|
As
VivoQuest is a development stage enterprise that had not yet commenced its
planned principal operations, the Company accounted for the Transaction as
an
acquisition of assets pursuant to the provisions of FAS No. 142 “Goodwill and
Other Intangible Assets.” Accordingly, the purchase price was allocated to the
individual assets acquired, based on their relative fair values, and no goodwill
was recorded.
The
purchase price consisted of:
|
($
in thousands)
|
||||
|
Fair
value of the Company’s ordinary shares
|
1,391
|
|||
|
Cash
consideration paid
|
400
|
|||
|
Direct
expenses associated with the Transaction
|
148
|
|||
|
Total
purchase price
|
1,939
|
|||
F-22
XTL
BIOPHARMACEUTICALS LTD.
(A
Development Stage Company)
NOTES
TO
THE CONSOLIDATED FINANCIAL STATEMENTS (continued)
NOTE
3 - LICENSE AND ASSET PURCHASE AGREEMENT WITH VIVOQUEST
(continued):
The
tangible and intangible assets acquired consisted of the following:
|
($
in thousands)
|
||||
|
Tangible
assets acquired - property and equipment
|
113
|
|||
|
Intangible
assets acquired:
|
||||
|
In-process
research and development
|
1,783
|
|||
|
Assembled
workforce
|
43
|
|||
|
Total
intangible assets acquired
|
1,826
|
|||
|
Total
tangible and intangible assets acquired
|
1,939
|
|||
The
fair
value of the in-process research and development acquired was estimated by
management with the assistance of an independent third-party appraiser, using
the ”income approach.” In the income approach, fair value is dependent on the
present value of future economic benefits to be derived from ownership of an
asset. Central to this approach is an analysis of the earnings potential
represented by an asset and of the underlying risks associated with obtaining
those earnings. Fair value is calculated by discounting future net cash flows
available for distribution to their present value at a rate of return, which
reflects the time value of money and business risk. In order to apply this
approach, the expected cash flow approach was used. Expected cash flow is
measured as the sum of the average, or mean, probability-weighted amounts in
a
range of estimated cash flows. The expected cash flow approach focuses on the
amount and timing of estimated cash flows and their relative probability of
occurrence under different scenarios. The probability weighted expected cash
flow estimates are discounted to their present value using the risk free rate
of
return, since the business risk is incorporated in adjusting the projected
cash
flows to the probabilities for each scenario. The risk-free discount rate
assumed for the valuation of the license to the intellectual property is 4.6%,
based upon the yields on long-term U.S. treasury securities, as of the valuation
date.
The
fair
value of the assembled workforce acquired was estimated by management with
the
assistance of an independent third-party appraiser, based upon the cost
approach. The cost approach measures the fair- value based on the cost of
reproducing or replacing an asset, less depreciation and amortization from
physical deterioration and functional or economic obsolescence, if present
and
measurable. According to this approach, the estimated fair-value of the
assembled workforce is based on the cost of replacing VivoQuest’s key employees,
which were hired by the Company as a part of Transaction.
The
amount allocated to in-process research and development represents the relative
fair value of purchased in-process research and development that, as of the
transaction date, have not reached technological feasibility and have no proven
alternative future use. Accordingly, they were charged in the consolidated
statement of operations as “in- process research and development
costs.”
The
assembled workforce that was acquired is being amortized using the straight-line
method over its estimated useful life of three years, and is classified as
“intangible assets” on the Company’s balance sheet.
F-23
XTL
BIOPHARMACEUTICALS LTD.
(A
Development Stage Company)
NOTES
TO
THE CONSOLIDATED FINANCIAL STATEMENTS (continued)
NOTE
3 - LICENSE AND ASSET PURCHASE AGREEMENT WITH VIVOQUEST
(continued):
For
the
year ended December 31, 2005, amortization of the assembled workforce was
$4,000. Estimated amortization expenses of the assembled workforce for future
years subsequent to December 31, 2005 are $14,000 for 2006 and 2007, and
$11,000 for 2008.
NOTE
4 - PROPERTY AND EQUIPMENT:
|
a.
|
Composition
of the assets, grouped by major classifications, is as
follows:
|
|
December
31
|
|||||||
|
2005
|
2004
|
||||||
|
($
in thousands)
|
|||||||
|
Property
and equipment
|
|||||||
|
Cost:
|
|||||||
|
Laboratory
equipment
|
1,960
|
1,828
|
|||||
|
Computers
|
232
|
517
|
|||||
|
Leasehold
improvements
|
698
|
698
|
|||||
|
Furniture
and office equipment
|
238
|
269
|
|||||
|
3,128
|
3,312
|
||||||
|
Accumulated
depreciation and amortization:
|
|||||||
|
Laboratory
equipment
|
1,333
|
1,120
|
|||||
|
Computers
|
217
|
488
|
|||||
|
Leasehold
improvements
|
697
|
691
|
|||||
|
Furniture
and office equipment
|
119
|
105
|
|||||
|
2,366
|
2,404
|
||||||
|
762
|
908
|
||||||
|
b.
|
Under
the provisions of FAS 144, the Company’s management reviewed the carrying
value of certain laboratory equipment, and recorded an impairment
charge
in an amount of $ 26,000 in 2005. See Note 9.
During
2003, the Company’s management determined to put on hold early-stage
research activities, and consequently, to sell an asset used in one
of
these activities. Under the provisions of FAS 144, the Company’s
management reviewed the carrying value of this asset (original cost
$ 415,000, depreciated amount - $ 354,000) and determined to
write it off. An impairment charge in an amount of $ 354,000 was
recorded.
|
|
c.
|
Depreciation
totaled $ 238,000, $ 319,000 and $ 440,000 for the years ended December
31, 2005, 2004 and 2003,
respectively.
|
F-24
XTL
BIOPHARMACEUTICALS LTD.
(A
Development Stage Company)
NOTES
TO
THE CONSOLIDATED FINANCIAL STATEMENTS (continued)
NOTE
5 - EMPLOYEE
SEVERANCE OBLIGATIONS:
| a. |
The
Company
|
Israeli
labor law generally requires payment of severance upon dismissal of an employee
or upon termination of employment in certain other circumstances. The following
principal plans relate to the Company:
| 1) |
On
June 30, 2001, the Company entered into an agreement with each employee
implementing Section 14 of the Severance Compensation Act, 1963 (the
“Law”) and the General Approval of the Labor Minister issued in accordance
to the said Section 14, mandating that upon termination of such employee’s
employment, the Company shall release to the employee all the amounts
accrued in its insurance policies. Accordingly, the Company remits
each
month to each of its employee’s insurance policy, the amounts required by
the law to cover the severance pay liability.
The
employee severance obligations covered by these contribution plans
are not
reflected in the financial statements, as the severance payment obligation
has been irrevocably transferred to the severance
funds.
|
| 2) |
Insurance
policies for certain employees (senior managers): the policies provide
most of the coverage for severance pay and pension liabilities of
managerial personnel, the remainder of the liabilities are covered
by the
Company.
The
Company has recorded an employee severance obligation for the amount
that
would be paid if all those employees were dismissed at the balance
sheet
date, on an undiscounted basis, in accordance with Israeli labor
law. This
liability is computed based upon the number of years of service
multiplied
by the latest monthly salary. The amount of accrued severance represents
the Company’s severance obligation in accordance with labor agreements in
force and based on salary components, which in management’s opinion,
create an entitlement to severance.
The
Company may only utilize the severance pay funds in the insurance
policies
for the purpose of disbursement of
severance.
|
| b. |
The
Subsidiary
The
Subsidiary’s severance obligation is calculated based on the employment
agreements between the Subsidiary and its employees.
|
| c. |
Severance
expenses
Severance
expenses (income) totaled $ (159,000), $ 30,000 and $ 129,000
for the
years ended December 31, 2005, 2004 and 2003, respectively.
Loss
(gain) on employee severance pay funds in respect of employee
severance
obligations totaled $(6,000), $(4,000), and $5,000 for the years
ended
December 31, 2005, 2004 and 2003, respectively.
|
F-25
XTL
BIOPHARMACEUTICALS LTD.
(A
Development Stage Company)
NOTES
TO
THE CONSOLIDATED FINANCIAL STATEMENTS (continued)
NOTE
5 - EMPLOYEE RIGHTS UPON RETIREMENT (continued):
|
d.
|
Cash
flow information regarding the Company’s liability for employee rights
upon retirement:
|
| 1) |
The
Company contributed in 2005, 2004 and 2003 to the insurance companies,
in
respect to its severance obligations to Israeli employees, $166,000,
$276,000 and $348,000, respectively, and expects to contribute, in
2006, $
90,000 to the insurance companies in respect to its severance obligations
to Israeli employees.
|
| 2) |
The
Company expects to pay future benefits to certain employees who will
reach
retirement, as follows:
|
|
($
in thousands)
|
|
|
2010
|
9
|
|
2011-2015
|
59
|
|
68
|
The
above
amounts were determined based on the employees’ current salary of the employees
and the number of service years that will be accumulated upon their retirement
date. These amounts do not include amounts that might be paid to employees
that
will cease being employed by the Company prior to the normal retirement age.
NOTE
6 - SHAREHOLDERS’ EQUITY:
|
a.
|
Share
Capital
As
of December 31, 2005, the Company’s ordinary shares are traded on the
London Stock Exchange (“LSE”) and on the Tel Aviv Stock Exchange (“TASE”).
The closing price per share, as of December 31, 2005 was 45p
on the LSE
($0.78) and NIS 3.64 on the TASE ($0.79). In addition, the Company’s
ADRs
trade on the Nasdaq National Market, with each ADR representing
ten
ordinary shares. The closing price of the Company’s ADRs, as of December
31, 2005, was $7.74
On
September 20, 2000 the Company completed an IPO, as result of
which
20,900,000 ordinary shares of NIS 0.02 each have been issued.
The proceeds
of the issuance of shares in the amount of ₤ 31.3 million (before
deduction of share issue expenses) were received as $ 44.7 million.
The
underwriters of the IPO were granted an over-allotment option.
Accordingly, on October 26, 2000, the Company issued 2,850,000
Ordinary
Shares of NIS 0.02 for a consideration of $ 6.2 million (before
deduction
of share issue expenses) at the price of ₤ 1.5 per share or $2.1 per share
(the IPO price) to meet over-allotments in connection with the
placing.
On
August 2, 2004, the Company completed a Placing and Open Offer
for new
ordinary shares, as result of which 56,009,732 Ordinary shares
of NIS 0.02
each have been issued. The gross proceeds of the issuance of
shares
amounted to ₤9.8 million - $17.8 million (approximately ₤8.5 million -
$15.4 million, net of issuance costs).
On
September 21, 2005, the Company issued to VivoQuest Inc. the
fair value
equivalent of $1,391,000 of its ordinary shares for a total of
1,314,420
ordinary shares (see Note 3).
|
F-26
XTL
BIOPHARMACEUTICALS LTD.
(A
Development Stage Company)
NOTES
TO
THE CONSOLIDATED FINANCIAL STATEMENTS (continued)
NOTE
6 - SHAREHOLDERS’ EQUITY
(continued):
|
b.
|
Stock
Option Plans:
|
|
1)
|
The
Company maintains the following share option plans for its employees,
directors and consultants.
The
Company’s board of directors administers its share option plans and has
the authority to designate all terms of the options granted under
the
Company’s plans including the grantees, exercise prices, grant dates,
vesting schedules and expiration dates, which may be no more than
ten
years after the grant date.
As
of December 31, 2005, the Company has granted to employees, directors
and
consultants options that are outstanding to purchase up to 24,793,975
ordinary shares, under the five share option plans discussed below
and
pursuant to certain grants apart from these plans also discussed
below.
|
|
(a)
|
1998
Share Option Plan
Under
a share option plan established in 1998, (“the 1998 Plan”), the Company
granted options to employees during 1998, which are held by a trustee
under section 3(i) of the Israeli tax ordinance, of which 3,884,810
are
outstanding and exercisable as of December 31, 2005 at an exercise
price
per share of $0.497.
The
option term is for a period of 10 years from grant date. If the options
are not exercised and the shares not paid for by such date, all interests
and rights of any grantee shall expire. These options were granted
for no
consideration. There are no options available for grant from this
plan.
|
|
(b)
|
1999
Share Option Plan
Under
a share option plan established in 1999, (“the 1999 Plan”), the Company
granted options to employees during 1999, which are held by a trustee
under section 3(i) of the Tax Ordinance, of which 955,920 are outstanding
and exercisable as of December 31, 2005, at an exercise price of
$0.497.
The
option term is for a period of 10 years from grant date. If the options
are not exercised and the shares not paid for by such date, all interests
and rights of any grantee shall expire. These options were granted
for no
consideration. There are no options available for grant from this
plan.
|
|
(c)
|
1999
International Share Option Plan
Under
an international share option plan established in 1999, (“the
International Plan”), the Company granted options to employees during 1999
and 2000, of which 1,380,000 are outstanding and exercisable as of
December 31, 2005, at an exercise price between $0.497 and $1.10.
|
F-27
XTL
BIOPHARMACEUTICALS LTD.
(A
Development Stage Company)
NOTES
TO
THE CONSOLIDATED FINANCIAL STATEMENTS (continued)
NOTE
6 - SHAREHOLDERS’ EQUITY
(continued):
|
|
The
options granted thereunder are outstanding and exercisable until
October
2007. If the options are not exercised and the shares are not paid
for by
such date, all interests and rights of any grantee shall expire.
These
options were granted for no consideration. There are no options
available
for grant from this plan.
|
|
(d)
|
2000
Share Option Plan
Under
a share option plan established in 2000, (“the 2000 Plan”), the Company
granted options to employees during 2000, which are held by a
trustee
under section 3(i) of the Tax Ordinance, of which 855,300 are
outstanding
and exercisable as of December 31, 2005, at an exercise price
of $1.10.
The
option term is for a period of 10 years from grant date. If the
options
are not exercised and the shares not paid for by such date, all
interests
and rights of any grantee shall expire. These options were granted
for no
consideration. There are no options available for grant from
this plan.
|
|
(e)
|
2001
Share Option Plan
Under
a share option plan established in 2001, (“the 2001 Plan”), the Company
granted options to employees during
2001-2004,
including directors, according to which up to 11,000,000 options
were
available to be granted, of which 2,703,485 are outstanding as
of December
31, 2005, at an exercise price per share between $0.106 and $0.931.
These
options were granted in accordance with section 102 of the Tax
Ordinance,
under the capital gains option set out in section 102(b)(2) of
the
ordinance.
The
option term is for a period of 10 years from grant date.
The options were granted for no consideration. The options vest
over a
four year period, with vesting occurring on the 2nd, 3rd and
4th
anniversary from the grant date, and in addition, the lock up
period of
the options is for two years from the date of grant. Compensation
expenses
are calculated based on the straight line method. As of December
31, 2005,
2,316,820 options are fully vested. As of December 31, 2005,
the remaining
number of options available for future grants in this pool is
7,919,960.
|
|
(f)
|
Non-Plan
Share Options
In
addition to the options granted under the Company’s share option plans,
there are 15,014,460 outstanding options, and 7,224,460 exercisable
options, as of December 31, 2005, which were granted by the Company
to
employees, directors and consultants not under an option plan
during
1997-2005.
The options were granted at an exercise price per share between
$0.20 and
$2.11. The options expire between 2007 and 2015. The options
which were
granted during 2005, are from the Non-Plan
Share Options, see 2(a) and 2(b) below for the term of the options.
|
F-28
XTL
BIOPHARMACEUTICALS LTD.
(A
Development Stage Company)
NOTES
TO
THE CONSOLIDATED FINANCIAL STATEMENTS (continued)
NOTE
6 - SHAREHOLDERS’ EQUITY
(continued):
|
2)
|
The
following table summarizes options granted to employees and directors
under the Company's stock option plans, as discussed
above:
|
|
Year
ended December 31
|
|||||||||||||||||||
|
2005
|
2004
|
2003
|
|||||||||||||||||
|
Weighted
|
Weighted
|
Weighted
|
|||||||||||||||||
|
Average
|
average
|
average
|
|||||||||||||||||
|
Number
|
exercise
price
|
Number
|
exercise
price
|
Number
|
exercise
price
|
||||||||||||||
|
$
|
$
|
$
|
|||||||||||||||||
|
Balance
outstanding at
|
|||||||||||||||||||
|
beginning
of year
|
17,805,661
|
0.69
|
17,552,661
|
0.69
|
19,891,823
|
0.71
|
|||||||||||||
|
Changes
during the year:
|
|||||||||||||||||||
|
Granted
*
|
11,370,000
|
0.36
|
432,000
|
0.33
|
824,900
|
0.13
|
|||||||||||||
|
Exercised
**
|
(3,786,825
|
)
|
0.40
|
(50,000
|
)
|
0.37
|
(854,100
|
)
|
0.01
|
||||||||||
|
Expired
and forfeited
|
(1,119,861
|
)
|
0.47
|
(129,000
|
)
|
0.68
|
(2,309,962
|
)
|
0.87
|
||||||||||
|
Balance
outstanding at
|
|||||||||||||||||||
|
end
of year***
|
24,268,975
|
0.59
|
17,805,661
|
0.69
|
17,552,661
|
0.69
|
|||||||||||||
|
Balance
exercisable at end
|
|||||||||||||||||||
|
of
year***
|
16,262,310
|
0.70
|
16,051,324
|
0.72
|
11,924,323
|
0.63
|
|||||||||||||
*
In
2004
and 2003, the options exercise price was equal to the share price on the grant
date. In 2005, the options exercise price for two directors was below the share
price on the grant date, and for two other directors the options exercise price
was equal to the share price on the grant date. See (a) and (b) below.
**
The
total intrinsic value of options exercised during 2005, 2004 and 2003 is
$1,521,000, $6,000 and $123,000, respectively.
***
The
aggregate intrinsic value as of December 31, 2005 is $7,293,000 for outstanding
options, and $3,882,000 for exercisable options.
|
|
The
following table summarizes information about stock options granted
to
employees and directors outstanding and exercisable at December 31,
2005:
|
|
Options
outstanding
|
Options
exercisable
|
||||||||||||
|
Weighted
|
Weighted
|
||||||||||||
|
average
|
average
|
||||||||||||
|
Balance
at
|
remaining
|
|
Balance
at
|
remaining
|
|||||||||
|
December 31,
|
|
contractual
|
|
December 31,
|
contractual
|
||||||||
|
2005
|
life
|
2005
|
life
|
||||||||||
|
Number
|
In
years
|
Number
|
In
years
|
||||||||||
|
Exercise
prices:
|
|||||||||||||
|
$
0.106
|
355,523
|
6.4
|
102,658
|
4.4
|
|||||||||
|
$
0.250
|
125,000
|
7.7
|
41,667
|
7.7
|
|||||||||
|
$
0.315
|
6,200
|
1.0
|
6,200
|
1.0
|
|||||||||
|
$
0.354
|
11,250,000
|
4.6
|
3,750,000
|
4.6
|
|||||||||
|
$
0.365
|
1,045,120
|
1.1
|
1,045,120
|
1.1
|
|||||||||
|
$
0.482
|
19,600
|
4.2
|
15,600
|
3.5
|
|||||||||
|
$
0.486
|
9,900
|
0.6
|
9,900
|
0.6
|
|||||||||
|
$
0.497
|
6,180,070
|
2.5
|
6,180,070
|
2.5
|
|||||||||
|
$
0.766
|
108,800
|
5.1
|
108,800
|
5.1
|
|||||||||
|
$
0.851
|
150,200
|
5.8
|
103,733
|
5.6
|
|||||||||
|
$
0.853
|
120,000
|
9.6
|
—
|
—
|
|||||||||
|
$
0.931
|
1,928,262
|
4.1
|
1,928,262
|
4.1
|
|||||||||
|
$
1.10
|
1,695,300
|
3.0
|
1,695,300
|
3.0
|
|||||||||
|
$
2.110
|
1,275,000
|
4.7
|
1,275,000
|
4.7
|
|||||||||
|
|
24,
268,975
|
3.9
|
16,262,310
|
3.4
|
|||||||||
F-29
XTL
BIOPHARMACEUTICALS LTD.
(A
Development Stage Company)
NOTES
TO
THE CONSOLIDATED FINANCIAL STATEMENTS (continued)
NOTE
6 - SHAREHOLDERS’ EQUITY (continued):
|
(a)
|
In
August 2005, the Company’s shareholders granted its Chairman of the Board
(the “Chairman”) and one of its non-executive directors, options to
purchase a total of 9,250,000 and 2,000,000 ordinary shares,
respectively,
at an exercise price equal to $0.354 per share (which was below
market
price) . These options are exercisable for a period of five
years from the
date of issuance, and granted under the same terms and conditions
as the
2001 Plan. The options shall vest upon achievement of certain
market
conditions (each 1/3 of the options will vest upon achievement
of a
certain market condition). In addition, with regard to the
Chairman, in
the event of a merger, acquisition or other change of control
or in the
event that the Company terminates the Chairman, either without
cause or as
a result of his death or disability, or he terminates his agreement
for
good reason, the exercisability of any of the options granted
to him
(9,250,000 options) that are unexercisable at the time of such
event or
termination shall accelerate and the time period during which
he shall be
allowed to exercise such options shall be extended by two years
from the
date of the termination of his agreement. Additionally, the
Company’s
board of directors shall have the discretion to accelerate
all or a
portion of the Chairman’s options at any time. As of December 31, 2005,
3,083,333 options that were granted to the Chairman and 666,667
options
that were granted to one of its non-executive directors are
vested (the
first milestone was reached and therefore 1/3 of the options
were vested).
The compensation expenses are amortized using the graded method.
The
Company used a lattice model that incorporated a Monte Carlo
Simulation
method as the fair value option pricing model, which was
estimated by
management with the assistance of an independent third-party
appraiser.
The following assumptions under this method were used for
the stock
options granted: risk free interest rate of 4.6% (in dollar
terms),
expected volatility of 50%, dividend yield of 0%, and derived
expected
life of 1.43 to 4.37 years. The weighted average fair value
of options
granted during the year, estimated by using the Monte Carlo
Simulation
Method was $0.53 per option.
|
|
(b)
|
In
August 2005, the Company granted to two of its
non-executive directors a grant of 60,000 options each, having
an exercise
price equal to $0.853 per share (which was at market price),
vesting over
the three years from the date of grant. In addition, they also
provided
for an annual grant of 20,000 options each, for three years,
at an
exercise price equivalent to the then current closing price of
the
Company’s ADR’s on the Nasdaq National Market. The future grants are
contingent on them being members of the board of directors at
such time.
The
Company used a Black & Scholes model as the fair value option pricing
model. The following assumptions under the Black & Scholes model were
used for the stock option granted: expected
volatility of: 50%; risk-free interest rates (in dollar terms)
of: 4.6%,
dividend yield of 0% and expected life of 5 years (based on
management
estimation).
The
weighted average fair value of options using the Black & Scholes
model, granted during the year, estimated by using the model
was $0.42 per
option.
|
F-30
XTL
BIOPHARMACEUTICALS LTD.
(A
Development Stage Company)
NOTES
TO
THE CONSOLIDATED FINANCIAL STATEMENTS (continued)
NOTE
6 - SHAREHOLDERS’ EQUITY (continued):
|
(c)
|
The
weighted average fair value of options granted during 2004
and 2003,
estimated by using the Black & Scholes option-pricing model, was $
0.10 and $ 0.07 for the year ended December 31, 2004, and
2003,
respectively. The fair value of options was estimated on
the date of
grant, based on the following weighted average assumptions:
dividend yield
of 0% for all relevant years; expected volatility of: 2004
- 35% and 2003
- 45%; risk-free interest rates (in dollar terms) of: 2004
- 2.9% and 2003
- 2.75%; and expected life of 2 to 4 years, for each of the
reported
years, depending on the vesting period of the options.
|
|
(d)
|
The non-cash compensation relating to options granted to employees and directors were $2,718,000 in 2005 (of which $67,000 was charged to research and development costs, $2,641,000 was charged to general and administrative expenses and $10,000 was charged to business development costs.). The total compensation costs related to nonvested awards not recognized as of December 31, 2005 is $3,408,000, and the weighted average period over which it is expected to be recognized is 3.6 years. |
|
3)
|
The
following table summarizes options granted to consultants (including
consultants and members of the scientific advisory board and
other
third-party service providers) under the Company's stock option
plans, as
discussed above:
|
|
Year
ended December 31
|
|||||||||||||||||||
|
2005
|
2004
|
2003
|
|||||||||||||||||
|
Weighted
|
Weighted
|
Weighted
|
|||||||||||||||||
|
average
|
average
|
average
|
|||||||||||||||||
|
Number
|
exercise
price
|
Number
|
exercise
price
|
Number
|
exercise
price
|
||||||||||||||
|
$
|
$
|
$
|
|||||||||||||||||
|
Balance
outstanding at beginning of year
|
525,000
|
0.33
|
205,000
|
0.54
|
205,000
|
0.54
|
|||||||||||||
|
Changes
during the year - granted*
|
—
|
—
|
320,000
|
0.20
|
—
|
—
|
|||||||||||||
|
Balance
outstanding at end of year**
|
525,000
|
0.33
|
525,000
|
0.33
|
205,000
|
0.54
|
|||||||||||||
|
Balance
exercisable at end of year**
|
355,000
|
0.39
|
280,901
|
0.45
|
205,000
|
0.54
|
|||||||||||||
| * |
The
options exercise price was equal to the share price on the grant
date.
|
| ** | The aggregate intrinsic value as of December 31, 2005 is $236,000 for outstanding options, and $137,000 for exercisable options. |
F-31
XTL
BIOPHARMACEUTICALS LTD.
(A
Development Stage Company)
NOTES
TO
THE CONSOLIDATED FINANCIAL STATEMENTS (continued)
NOTE
6 - SHAREHOLDERS’ EQUITY (continued):
The
following table summarizes information about stock options outstanding and
exercisable at December 31, 2005:
|
Options
outstanding
|
Options
exercisable
|
||||||||||||
|
Weighted
|
|
Weighted
|
|||||||||||
|
average
|
|
average
|
|||||||||||
|
Balance
at
|
remaining
|
Balance
at
|
remaining
|
||||||||||
|
December 31,
|
contractual
|
December 31,
|
contractual
|
||||||||||
|
2005
|
life
|
2005
|
life
|
||||||||||
|
Number
|
In
years
|
Number
|
In
years
|
||||||||||
|
Exercise
prices:
|
|||||||||||||
|
$
0.20
|
150,000
|
2.7
|
150,000
|
2.7
|
|||||||||
|
$
0.20
|
170,000
|
*
|
—
|
—
|
|||||||||
|
$
0.497
|
10,000
|
3.4
|
10,000
|
3.4
|
|||||||||
|
$
0.538
|
195,000
|
1.0
|
195,000
|
1.0
|
|||||||||
|
525,000
|
355,000
|
||||||||||||
|
*
Two years from date of regulators approval to sell in any geographic
location. The options were granted during 2004.
|
|||||||||||||
|
(a)
|
The
Company used the Black & Scholes fair value option pricing model. The
following assumptions under this method were used in 2005:
expected
volatility of 50%, risk free interest rates (in dollars
terms) of 4.6% and
expected life of three years. The following assumptions
under this method
were used in 2004: expected volatility of 33%, risk free
interest rates
(in dollars terms) of 3.6% and expected life of five years.
The weighted
average fair value of options granted during 2004, estimated
by using the
Black & Scholes fair value option pricing model was $0.30 for 2004,
and $0.88 per option for 2005.
|
|
(b)
|
The
non-cash compensation relating to options granted to consultants
were
$45,000 in 2005 and were charged to research and development
costs. The
charges for non-cash compensation relating to options granted
to
consultants were $32,000 in 2004 (of which $30,000 was
charged to research
and development costs, and $2,000 was charged to general
and
administrative expenses). There is no compensation costs
related to
nonvested awards not recognized as of December 31,
2005.
|
XTL
BIOPHARMACEUTICALS LTD.
(A
Development Stage Company)
NOTES
TO
THE CONSOLIDATED FINANCIAL STATEMENTS (continued)
NOTE
7 - COMMITMENTS AND CONTINGENCIES:
|
a.
|
Royalty
Bearing Agreements:
|
| 1) |
Under
a Research and License agreement with Yeda Research and Development
Company Ltd. (“Yeda”), the Company is committed to pay royalty payments at
rates determined in the agreement not exceeding 3% of net sales,
or
royalty rates mainly between 20% to 25% of sublicensing fees, for
products
in development and research under such an agreement.
The
Company has entered into certain license agreements with third
parties in
respect of particular projects. In connection with such agreements,
the
Company may incur royalty and milestone obligations commitments
at varying
royalty rates not exceeding 5 % of future net sales or 25 % of
sublicensing fees of products developed, based on such agreements.
Additionally,
the Company has undertaken to make contingent milestone payments
to
certain licensors of up to approximately $49.0 million over the
life of
the licenses, of which $34.0 million will be due upon or following
regulatory approval of the drugs (for contingent milestones related
to
VivoQuest’s purchase agreement which are included in these figures, see
Note 3).
In
some cases, these contingent milestone payments will only be
triggered
upon receipt of royalties on sales of related products and in
certain
cases will partially offset royalties the Company would otherwise
owe
those
licensors.
In addition, the Company is required to pay one of its licensors
an amount
of $100,000-$200,000 per year, as minimum royalties, during the
life of
the license. The Company may terminate at any time the agreement
with the
licensor upon advance notice of six months.
|
| 2) |
The
Company is committed to pay royalties to the Government of Israel
on
proceeds from sales of products in the research and development
of which
the Government participates by way of grants. At the time grants
were
received, successful development of the related projects was not
assured.
In the case of failure of a project that was partly financed as
above, the
Company is not obligated to pay any such royalties. Under the terms
of
Company's funding from the Israeli Government, royalties of 3%
- 5% are
payable on sales of products developed from projects so funded,
up to 100%
of the amount of the grant received by the Company (dollar linked);
as
from January 1, 1999 - with the addition of an annual interest
based on
Libor.
At
December 31, 2005, the maximum amount of the contingent liability
in
respect of royalties related to ongoing projects to the government
is
$3,778,000.
|
F-33
XTL
BIOPHARMACEUTICALS LTD.
(A
Development Stage Company)
NOTES
TO
THE CONSOLIDATED FINANCIAL STATEMENTS (continued)
NOTE
7 - COMMITMENTS AND CONTINGENCIES
(continued):
|
In
addition, the Company has received the approval of the Government
of Israel for the transfer of manufacturing rights of its HepeX-B
product,
under the terms of the agreement with Cubist (see Note 2). As
a
consequence, thereof, the Company is obligated to repay the grants
received from the
Government
of Israel for the financing of the HepeX-B product from any amounts
received by the Company from Cubist due to the sales of HepeX-B
product,
at a percentage rate, per annum, calculated based on the aggregate
amount
of grants received from the Government
of Israel divided by all amounts invested by the Company in the
research
and development activities of HepeX-B, and up to an aggregate
amount of
300% of the original amounts received for such project, including
interest
at the Libor rate. As of December 31, 2005, the aggregate amount
received
from the
Government
of Israel for the financing of the HepeX-B project including
interest and
Libor rate is equal to $4,213,000.
|
| 3) |
The
Company provided for annual
grants, over three years, of options to two of its non-executive
directors. The future grants are contingent on them being
members of the
board of directors at such time (see note
6(b)2b).
|
|
b.
|
Operating
lease
commitments:
|
| 1) |
The
Company leases its office space under lease agreements
that expire through
2009.
Future
minimum rental payments under these agreements are as
follows:
|
|
December
31, 2005
|
|
|
($
in thousands)
|
|
In
2006
|
667
|
|
In
2007
|
437
|
|
In
2008
|
450
|
|
In
2009
|
426
|
|
1,980
|
|
To
secure the lease agreement in Israel, the Company provided
a bank
guarantee. As of December 31, 2005, the guarantee is
secured by a pledge
on a long-term deposit amounting to $110,000 (December
31, 2004- $113,000)
linked to the Israeli Consumer Price Index (“CPI”), which is included in
the balance sheet as long-term deposit.
Rental
expenses for the years ended December 31, 2005, 2004
and 2003 were
$524,000, $394,000 and $427,000, respectively. The Company
has an option
to extend certain rental agreements for up to 5 years.
|
F-34
XTL
BIOPHARMACEUTICALS LTD.
(A
Development Stage Company)
NOTES
TO
THE CONSOLIDATED FINANCIAL STATEMENTS (continued)
NOTE
7 - COMMITMENTS AND CONTINGENCIES (continued):
| 2) |
The
Company leases vehicles under the terms of certain
operating lease
agreements that expire through 2007. Future minimum
lease payments -
linked to the CPI - are as
follows:
|
|
December
31, 2005
|
|
|
($
in thousands)
|
|
In
2006
|
53
|
|
In
2007
|
34
|
|
87
|
|
Vehicle
lease expense for the years ended December 31, 2005,
2004 and 2003 were
$76,000, $84,000 and $105,000, respectively.
|
|
c.
|
Research
and development agreement commitments
The
Company has commitments to pay amounts aggregating $ 652,000,
in respect
of research and development costs (mainly to outside service
providers),
of which $585,000 relates to 2006 and $67,000 relates to
2007.
|
|
d.
|
Tax
Assessment
In
2005, the Company received an assessment from the Israeli
tax authorities
of approximately $730,000 (including fines and interest
expenses) related
to withholding taxes for the periods of 2001-2004. The
Company has
recorded an accrual to reflect the probable liability
associated with this
assessment, based on the opinion of management, which
is included as part
of general and administrative expenses.
|
NOTE
8 - INCOME TAXES:
|
a.
|
The
Company
Measurement
of results for tax purposes under the Income Tax (Inflationary
Adjustments) Law, 1985
Under
this law, results for tax purposes are measured in real
terms, having
regard to the changes in the CPI. The Company is taxed
under this
law.
Results
for tax purposes are measured on a real basis - adjusted
to reflect the
increase in the Israeli consumer price index (hereafter
- the CPI). As
explained in Note 1b, the financial statements are presented
in dollars.
The difference between the change in the Israeli CPI and
the NIS-dollar
exchange rate - both on annual and cumulative basis - causes
a difference
between taxable income and income reflected in these financial
statements
(see also Note
1i).
|
XTL
BIOPHARMACEUTICALS LTD.
(A
Development Stage Company)
NOTES
TO
THE CONSOLIDATED FINANCIAL STATEMENTS (continued)
NOTE
8 - INCOME TAXES (continued):
|
|
Tax
benefits under the Israeli Law for Encouragement of
Capital Investments,
1959
The
Company has been granted an “approved enterprise” status under the Israeli
Law for Encouragement of Capital Investments, 1959.
Income derived from
the approved enterprise during a period of 7 years
from the year in which
this enterprise first realizes taxable income, provided
the maximum period
to which it is restricted by the law has not elapsed,
is entitled to tax
benefits as follows:
Tax
exemption for two years and reduced tax rate for the
remaining eight
years. The Company has not yet incurred taxable income.
The reduced tax
rate is dependent upon the percentage of foreign-owned
holdings (10% -
25%). Since the Company is currently over 25% foreign
owned, it is
entitled to reduced tax rate of 25% .
The
Company has an “approved enterprise” plan from 2001. The expiration of
this plan is in 2015.
If
the Company subsequently
pays a dividend out of income derived from the “approved enterprise”
during the tax exemption period, it will be subject
to tax on the amount
distributed, including any company tax on these amounts,
at the rate which
would have been applicable had such income not been
exempt (25%).
The
entitlement to the above benefits is conditional upon
the Company
fulfilling the conditions stipulated by the law, regulations
published
there-under and the instruments of approval for the
specific investment in
approved enterprise. In the event of failure to comply
with these
conditions, the benefits may be cancelled and the Company
may be required
to refund the amount of the benefits, in whole or in
part, with the
addition of interest. The
Investment center is currently reviewing the Company’s final
implementation report and as a result, the Company
has not yet received a
final implementation approval with respect to its “approved enterprise”
from the Investment Center. Additionally, given the
Company’s significant
amount of net-operating losses and the limitation mentioned
above to the
benefit period, there is no certainty, if and when
the Company would be
able to enjoy the tax benefits described above.
Tax
benefits under the Israeli law for the Encouragement
of Industry
(Taxation), 1969
The
Company qualifies as “industrial company” under the above law. In
accordance with this law the Company is entitled
to certain benefits
including accelerated depreciation on industrial
buildings and equipment,
a deduction of 12.5% per year of the purchase price
of a good-faith
acquisition of patent and certain other intangible
property
rights.
|
F-36
XTL
BIOPHARMACEUTICALS LTD.
(A
Development Stage Company)
NOTES
TO
THE CONSOLIDATED FINANCIAL STATEMENTS (continued)
NOTE
8 - INCOME TAXES (continued):
|
Tax
rates in Israel applicable to income from other
sources
The
income of the Company not eligible for “approved enterprise” benefits,
mentioned above (other than income from “approved enterprises”, see c.
below) is taxed at the regular rate. Through December 31, 2003,
the
corporate tax was 36%. The corporate tax rates for 2004 and thereafter
are
as follows: 2004 - 35%, 2005 - 34%, 2006 - 31%, 2007 - 29%, 2008
- 27%,
2009 - 26% and for 2010 and thereafter -
25%.
|
|
b.
|
The
Subsidiary
The
Subsidiary is taxed according to U.S. tax
laws.
|
|
c.
|
Current
tax losses for tax
purposes
|
| 1) |
Company
Income
tax of the Company is computed on the basis of the income
in Israeli
currency as determined for statutory purposes.
The
Company incurred losses for tax purposes from inception.
The
carryforward loss for tax purposes as of December 31, 2005
is
approximately $ 94 million (linked to the CPI), which may
be offset
against future taxable income generated from a business,
(including
capital gains from the sale of assets used in the business)
with no
expiration date.
|
| 2) |
Subsidiary
The
Subsidiary is remunerated under a cost plus agreement
with the Company.
The subsidiary has incurred taxable income and recorded
tax expenses and
is taxed under the applicable U.S. tax
laws.
|
|
|
The
following table summarizes the taxes on income for the Company
and its
subsidiary for 2005, 2004 and
2003:
|
|
2005
|
2004
|
2003
|
|||||||||||||||||
|
($
in thousands)
|
($
in thousands)
|
($
in thousands)
|
|||||||||||||||||
|
Company
|
Subsidiary
|
Company
|
Subsidiary
|
|
Company
|
Subsidiary
|
|||||||||||||
|
Net
income (loss) before
|
|||||||||||||||||||
|
income
taxes
|
(14,187
|
)
|
250
|
(16,582
|
)
|
158
|
(14,327
|
)
|
117
|
||||||||||
|
Income
Taxes
|
—
|
78
|
—
|
49
|
—
|
78
|
|||||||||||||
|
Net
income (loss) for the year
|
(14,187
|
)
|
172
|
(16,582
|
)
|
109
|
(14,327
|
)
|
39
|
||||||||||
F-37
XTL
BIOPHARMACEUTICALS LTD.
(A
Development Stage Company)
NOTES
TO
THE CONSOLIDATED FINANCIAL STATEMENTS (continued)
NOTE
8 - INCOME TAXES (continued):
|
d.
|
Deferred
income taxes
As
a result of the“approved
enterprise” status of the Company, the Company’s current tax rate is 0%,
and therefore no deferred tax assets have been included in these
financial
statements in respect of carryforward losses.
|
|
e.
|
Reconciliation
of the theoretical tax expense to actual tax expense
The
main reconciling item, between the statutory tax rate of the Company
and
the effective rate is the non-recognition of tax benefits from
carryforward
tax losses due to the uncertainty of the realization of such tax
benefits
(see above).
|
|
f.
|
Tax
assessments
|
|
1)
|
Income
taxes
The
Company received tax assessments for the years up to and including
the
1998 tax year.
The
Company’s tax returns until 2001are considered final. The Subsidiary has
not been assessed for tax purposes since
incorporation.
|
|
2)
|
Withholding
taxes - see Note 7d.
|
NOTE
9 - RESTRUCTURING:
|
a.
|
2005
Restructuring
In
2005, the Company implemented a restructuring plan designed to
focus its
resources on the development of its lead programs, with the goal
of moving
these programs through to clinical proof of concept. The 2005
restructuring included a 32 person reduction in the Company’s workforce,
31 of whom were in research and development and one of whom was
in general
and administrative. As part of the 2005 restructuring, the Company
took a
charge in 2005 of $168,000, relating to employee dismissal costs,
$163,000
of which was included in research and development costs and $5,000
of
which was included in general and administrative expenses.
As
of December 31, 2005, 28 employees have left the Company under
the 2005
restructuring plan and approximately $147,000 of dismissal costs
have been
paid. The other 4 employees left the Company in early 2006. As
of December
31, 2005, approximately $21,000 in employee dismissal obligations
are
included in accounts payable and accruals. The balance of these
obligations was paid in early 2006.
In
December 2005, as a result of the Company's restructuring, and
in
accordance with the provisions of FAS 144, the
Company reviewed the carrying value of certain lab equipment assets,
and
recorded an impairment charge in
research and development costs
in
an amount of $26,000 in 2005 (see also Note 4b).
|
F-38
XTL
BIOPHARMACEUTICALS LTD.
(A
Development Stage Company)
NOTES
TO
THE CONSOLIDATED FINANCIAL STATEMENTS (continued)
NOTE
9 - RESTRUCURING
(continued):
|
b.
|
2003
Restructuring
In
2003, the Company implemented and completed a restructuring plan.
As a
result of this restructuring, the Company ceased all early-stage
discovery
research activities related to infectious diseases. The 2003 restructuring
included a 20-person reduction in its workforce in Israel, 18 of
whom were
in research and development and two of whom were in general and
administrative. As part of the 2003 restructuring, the Company
took a
charge in 2003 of $74,000, relating to employee dismissal costs,
$58,000
of which was included in research and development costs and $16,000
of
which was included in general and administrative expenses. The
Company
paid all of these amounts in 2003. As part of the 2003 restructuring,
the
Company reevaluated its long-lived assets in accordance with FAS
No. 144,
and recorded a non-cash impairment charge of $354,000 of fixed
assets for
the year ended December 31, 2003 (see Note 4b).
|
NOTE
10 - SUPPLEMENTARY FINANCIAL STATEMENT INFORMATION:
|
a.
|
Short-term
bank deposits
The
deposits are denominated in dollars and bear a weighted average
annual
interest rate of 4.23 % as of December 31, 2005 (as of December
31, 2004 -
1.81%).
|
|
b.
|
Accounts
receivable - other:
|
|
December
31
|
|||||||
|
2005
|
2004
|
||||||
|
($
in thousands)
|
|||||||
|
Prepaid
expenses
|
285
|
165
|
|||||
|
Employees
|
75
|
24
|
|||||
|
Value
added tax authorities
|
17
|
101
|
|||||
|
Other
|
54
|
16
|
|||||
|
431
|
306
|
||||||
|
c.
|
Accounts
payable and
accruals:
|
|
Suppliers
|
655
|
1,108
|
|||||
|
Accrued
expenses
|
940
|
1,337
|
|||||
|
Institutions
and employees in respect of salaries
|
|||||||
|
and
related benefits
|
250
|
294
|
|||||
|
Provision
for vacation pay and recreation pay
|
160
|
385
|
|||||
|
Other
|
2
|
10
|
|||||
|
2,007
|
3,134
|
F-39
XTL
BIOPHARMACEUTICALS LTD.
(A
Development Stage Company)
NOTES
TO
THE CONSOLIDATED FINANCIAL STATEMENTS (continued)
NOTE
10 - SUPPLEMENTARY FINANCIAL STATEMENT INFORMATION (continued):
|
|
Statements
of operations:
|
|
d.
|
Research
and development
costs:
|
|
Period
from
|
|||||||||||||
|
March
9, 1993
|
|
||||||||||||
|
Year
ended December 31
|
to
December 31,
|
||||||||||||
|
2005
|
2004
|
2003
|
2005
|
||||||||||
|
($
in thousands)
|
|||||||||||||
|
Wages,
salaries and related benefits
|
|||||||||||||
|
(includes
non-cash compensation
|
|||||||||||||
|
of
$67 in 2005, and $0
|
|||||||||||||
|
in
2004 and 2003)
|
2,764
|
2,776
|
3,450
|
23,709
|
|||||||||
|
Outside
service providers
|
2,054
|
6,430
|
6,799
|
35,910
|
|||||||||
|
Lab
supplies
|
558
|
754
|
1,128
|
8,964
|
|||||||||
|
Consultants
(includes non-cash
|
|||||||||||||
|
compensation
of $45 in 2005,
|
|||||||||||||
|
$30
in 2004 and $0 in 2003)
|
531
|
549
|
494
|
3,725
|
|||||||||
|
Rent
and maintenance
|
752
|
725
|
866
|
4,756
|
|||||||||
|
Impairment
loss
|
26
|
354
|
380
|
||||||||||
|
Depreciation
and amortization
|
212
|
277
|
369
|
2,929
|
|||||||||
|
Other
|
416
|
474
|
562
|
2,517
|
|||||||||
|
7,313
|
11,985
|
14,022
|
82,890
|
||||||||||
|
e.
|
General
and administrative expenses:
|
|
|
|||||||||||||
|
Wages,
salaries and related benefits
|
|||||||||||||
|
(includes
non-cash compensation
|
|||||||||||||
|
of
$5 in 2005, and $0 in 2004
|
|||||||||||||
|
and
2003)
|
454
|
1,890
|
1,244
|
11,534
|
|||||||||
|
Corporate
communications
|
140
|
289
|
228
|
2,350
|
|||||||||
|
Professional
fees
|
890
|
647
|
564
|
4,405
|
|||||||||
|
Director
fees and related (includes
|
|||||||||||||
|
non-cash
compensation of $2,636
|
|||||||||||||
|
in
2005, and $0 in 2004 and 2003)
|
2,821
|
243
|
183
|
4,208
|
|||||||||
|
Rent
and maintenance
|
91
|
90
|
104
|
956
|
|||||||||
|
Communications
|
25
|
34
|
33
|
220
|
|||||||||
|
Depreciation
and amortization
|
30
|
42
|
70
|
619
|
|||||||||
|
Patent
registration fees
|
174
|
271
|
125
|
1,191
|
|||||||||
|
Other
|
832
|
628
|
554
|
3,529
|
|||||||||
|
5,457
|
4,134
|
3,105
|
29,012
|
||||||||||
|
f.
|
Business
development costs:
|
|
Wages,
salaries and related
|
|||||||||||||
|
benefits
(includes non-cash
|
|||||||||||||
|
compensation
of $10 in 2005,
|
|||||||||||||
|
and
$0 in 2004 and 2003)
|
171
|
410
|
408
|
2,672
|
|||||||||
|
Travel
|
22
|
36
|
136
|
764
|
|||||||||
|
Professional
fees
|
34
|
364
|
120
|
1,077
|
|||||||||
|
227
|
810
|
664
|
4,513
|
||||||||||
F-40
XTL
BIOPHARMACEUTICALS LTD.
(A
Development Stage Company)
NOTES
TO
THE CONSOLIDATED FINANCIAL STATEMENTS (continued)
NOTE
10 - SUPPLEMENTARY FINANCIAL STATEMENT INFORMATION (continued):
|
g.
|
Financial
income,
net:
|
|
March
9, 1993
|
|||||||||||||
|
Year
ended December 31
|
to
December 31,
|
||||||||||||
|
2005
|
2004
|
2003
|
2005
|
||||||||||
|
($
in thousands)
|
|||||||||||||
|
Financial
income:
|
|
||||||||||||
|
Interest
income
|
503
|
297
|
458
|
9,228
|
|||||||||
|
Foreign
exchange differences-gain
|
—
|
67
|
—
|
203
|
|||||||||
|
Gain
from available for sale securities
|
—
|
13
|
62
|
13
|
|||||||||
|
Other
|
—
|
—
|
—
|
156
|
|||||||||
|
503
|
377
|
520
|
9,600
|
||||||||||
|
Financial
expenses:
|
|||||||||||||
|
Foreign
exchange differences-loss
|
39 |
—
|
148 |
1,960
|
|||||||||
|
Interest
expense
|
—
|
—
|
374
|
||||||||||
|
Loss
from available for sale securities
|
—
|
—
|
—
|
14
|
|||||||||
|
Other
|
21
|
25
|
20
|
109
|
|||||||||
|
60
|
25
|
168
|
2,457
|
||||||||||
|
Financial
income, net
|
443
|
352
|
352
|
7,143
|
|||||||||
NOTE
10 - FINANCIAL INSTRUMENTS AND RISK MANAGEMENT:
|
a.
|
Linkage
terms of balances in non-dollars
currency:
|
|
1)
|
As
follows:
|
|
December 31,
2005
|
|||||||
|
Israeli
currency
|
Other
|
||||||
|
Unlinked
|
|||||||
|
($
in thousands)
|
|||||||
|
Assets
|
934
|
122
|
|||||
|
Liabilities
|
987
|
45
|
|||||
|
|
The
above balances do not include Israeli currency balances linked
to the
dollar.
|
XTL
BIOPHARMACEUTICALS LTD.
(A
Development Stage Company)
NOTES
TO
THE CONSOLIDATED FINANCIAL STATEMENTS (continued)
NOTE
10 - FINANCIAL INSTRUMENTS AND RISK MANAGEMENT (continued):
|
2)
|
Data
regarding the changes in the exchange rate of the dollar and the
Israeli
CPI:
|
|
Year
ended December 31
|
||||||||||
|
2005
|
2004
|
2003
|
||||||||
|
Devaluation
(evaluation) of the Israeli currency
against the dollar
|
6.85%
|
|
(1.6)%
|
|
(7.6)%
|
|
||||
|
Changes
in the Israeli CPI
|
2.4 %
|
|
1.2%
|
|
(1.9)%
|
|
||||
|
Exchange
rate of one dollar (at end of year)
|
NIS
4.603
|
NIS
4.308
|
NIS
4.379
|
|||||||
|
b.
|
Fair
value of financial instruments
The
financial instruments of the Company consist of non-derivative
assets and
liabilities, included in working capital.
In
view of their nature, the fair value of these financial instruments
is
usually identical or close to their carrying
value.
|
|
c.
|
Concentration
of credit risks
Most
of the Company’s cash and cash equivalents and bank deposits at the
balance sheet dates were deposited with Israeli banks. The
Company is of
the opinion that the credit risk in respect of those balances
is
remote.
|
NOTE
11 - SUBSEQUENT EVENT
During
March 2006, the Audit Committee and the Board of Directors of the Company
approved the grant to the CEO of 7,000,000 options, to the Chairman 9,898,719
options and to a non-executive director 750,000 options, to purchase ordinary
shares of the Company. All of such options are subject to vesting of which
one
third is based on service period, and the remainder is based on achievement
of
certain milestones linked to the Company’s valuation on the public markets. The
option grant to the Chairman and to the non-executive director is subject to
shareholder approval.
F-42
VIVOQUEST,
INC.
(A
DEVELOPMENT STAGE ENTERPRISE)
FINANCIAL
STATEMENTS
DECEMBER
31, 2004
AND
THE CUMULATIVE PERIOD FROM
SEPTEMBER
29, 1998 (INCEPTION)
TO JUNE 30, 2005
|
Page
|
|
|
F-44
|
|
|
Financial
Statements:
|
|
|
F-46
|
|
|
F-47
|
|
|
F-48
|
|
|
F-51
|
|
|
F-52
|
F-43
To
the Board of Directors and Stockholders of
VivoQuest,
Inc.
New
York, New York
We
have
audited the accompanying balance sheet of VIVOQUEST, INC. (A DEVELOPMENT
STAGE
ENTERPRISE) as at December 31, 2004, and the related statements of operations
and changes in redeemable preferred stock and stockholders’ deficiency and cash
flows for the year then ended. These financial statements are the responsibility
of the Company's management. Our responsibility is to express an opinion
on
these financial statements based on our audit.
We
conducted our audit in accordance with standards of the Public Company
Accounting Oversight Board (United States). Those standards require that
we plan
and perform the audit to obtain reasonable assurance about whether the financial
statements are free of material misstatement. An audit includes examining,
on a
test basis, evidence supporting the amounts and disclosures in the financial
statements. An audit also includes assessing the accounting principles used
and
significant estimates made by management, as well as evaluating the overall
financial statement presentation. We believe that our audit provides a
reasonable basis for our opinion.
In
our
opinion, the financial statements referred to above present fairly, in all
material respects, the financial position of VivoQuest, Inc. as at December
31,
2004 and the results of its operations and its cash flows for the year then
ended in conformity with generally accepted accounting principles in the
United
States.
The
accompanying financial statements have been prepared assuming that the Company
will continue as a going concern. As discussed in Note 2 to the financial
statements, the Company has limited capital resources and has suffered recurring
net losses and negative cash flows from operations since inception. These
conditions raise substantial doubt about its ability to continue as a going
concern. Management’s plans regarding this matter is also described in Note 2.
The financial statements do not include any adjustments that might result
from
the outcome of this uncertainty.
/s/
CORNICK, GARBER & SANDLER, LLP
New
York, New York
April
6, 2006
F-44
Report
of Independent Auditors
To the
Board
of Directors and Shareholders of VivoQuest, Inc.:
In
our
opinion, the statement of redeemable preferred stock and stockholders'
deficiency present fairly, in all material respects, the results of operations
of VivoQuest
Inc. ("VivoQuest") (a
development stage enterprise) for
the
period from September
29, 1998 (date of inception) to December 31, 2003 in conformity with
accounting
principles generally accepted in the United States of America. This financial
statement is the responsibility of VivoQuest's management; our responsibility
is
to express an opinion on this financial statement based on our
audit. We
conducted our audit of this statement in accordance with auditing standards
generally accepted in the United States of America, which require that
we plan
and perform the audit to obtain reasonable assurance about whether the
financial
statement is free of material misstatement. An audit includes examining,
on a
test basis, evidence supporting the amounts and disclosures in the financial
statement, assessing the accounting principles used and significant estimates
made by management, and evaluating the overall financial statement presentation.
We believe that our audit provides a reasonable basis for our
opinion.
The
statement of redeemable preferred stock and stockholders' deficiency of
VivoQuest for the period from September 29, 1998 (date of inception) to
December
31, 2003 has been prepared assuming that the Company will continue as a
going
concern. As discussed in Note 2, to the financial statements, the Company
has
limited capital resources and has suffered net losses and negative cash
flows
from operations since inception which raise substantial doubt about its
ability
to continue as a going concern. Management's plan in regard to this matter
is
also described in Note 2. The financial statement does not include adjustments
that might result from the outcome of this uncertainty.
/s/
PricewaterhouseCoopers LLP
New
York,
New York
June
10,
2004
|
VIVOQUEST,
INC.
|
|||
|
(A
DEVELOPMENT STAGE ENTERPRISE)
|
|||
|
June
30,
|
December
31,
|
||||||
|
ASSETS
|
2005
|
2004
|
|||||
|
(unaudited)
|
|||||||
|
Current
assets:
|
|||||||
|
Cash
and cash equivalents
|
$
|
764,359
|
$
|
1,069,640
|
|||
|
Prepaid
expenses and other current assets
|
93,174
|
74,317
|
|||||
|
Total
current assets
|
857,533
|
1,143,957
|
|||||
|
Fixed
assets, at cost, net of accumulated depreciation
|
|||||||
|
and
amortization
|
581,201
|
792,503
|
|||||
|
Security
deposits
|
14,740
|
44,740
|
|||||
|
Other
assets
|
24,925
|
24,924
|
|||||
|
Total
assets
|
$
|
1,478,399
|
$
|
2,006,124
|
|||
|
LIABILITIES,
REDEEMABLE CONVERTIBLE PREFERRED STOCK
AND
|
|||||||
|
STOCKHOLDERS'
DEFICIENCY
|
|||||||
|
Current
liabilities:
|
|||||||
|
Accounts
payable and accrued expenses
|
$
|
633,335
|
$
|
198,025
|
|||
|
Notes
payable
|
4,184,643
|
2,084,642
|
|||||
|
Total
liabilities
|
4,817,978
|
2,282,667
|
|||||
|
Redeemable
Preferred stock, $1.00 par value; 33,844,305 shares
authorized:
|
|||||||
|
Series
A Convertible Preferred stock, $1.00 par value; 471,145
|
|||||||
|
shares
designated, issued and outstanding in 2005 and 2004
|
|||||||
|
(at
liquidation value), respectively
|
684,430
|
667,942
|
|||||
|
Series
B Convertible Preferred stock, $1.00 par value; 1,904,762
|
|||||||
|
shares
designated; 1,904,762 shares issued and outstanding in
|
|||||||
|
2005
and 2004 (at liquidation value), respectively
|
7,005,166
|
6,830,164
|
|||||
|
Series
C Convertible Preferred stock, $.01 par value; 31,468,398
|
|||||||
|
shares
designated; 28,224,878 shares issued and outstanding
|
|||||||
|
in
2005 and 2004 (liquidation value $23,280,389)
|
17,330,482
|
16,803,278
|
|||||
|
Total
redeemable preferred stock
|
25,020,078
|
24,301,384
|
|||||
|
Stockholders'
deficiency:
|
|||||||
|
Common
stock, $0.01 par value; 49,400,000 shares authorized;
|
|||||||
|
shares
issued and outstanding 5,769,999 shares in 2005
|
|||||||
|
and
5,756,294 shares in 2004
|
57,700
|
57,563
|
|||||
|
Additional
paid-in capital
|
(2,154,423
|
)
|
(1,437,396
|
)
|
|||
|
Stock
subscription receivable
|
(117,378
|
)
|
(116,399
|
)
|
|||
|
Deficit
accumulated during the development stage
|
(26,145,556
|
)
|
(23,081,695
|
)
|
|||
|
Total
stockholders' deficiency
|
(28,359,657
|
)
|
(24,577,927
|
)
|
|||
|
Total
liabilities, redeemable convertible preferred
|
|||||||
|
stock
and stockholders' deficiency
|
$
|
1,478,399
|
$
|
2,006,124
|
|||
|
|
|||||||
|
The
notes to financial statements are made a part
hereof.
|
F-46
|
VIVOQUEST,
INC.
|
|||||||||
|
(A
DEVELOPMENT STAGE ENTERPRISE)
|
|||||||||
|
Cumulative
from
|
|||||||||||||
|
September
29, 1998
|
|||||||||||||
|
Six
Months Ended
|
Year
Ended
|
(inception)
to
|
|||||||||||
|
June
30,
|
December
31,
|
June
30,
|
|||||||||||
|
2005
|
2004
|
2004
|
2005
|
||||||||||
|
(unaudited)
|
(unaudited)
|
(unaudited)
|
|||||||||||
|
Operating
expenses:
|
|||||||||||||
|
Research
and development
|
$
|
2,051,705
|
$
|
1,715,119
|
$
|
3,430,162
|
$
|
14,284,983
|
|||||
|
General
and administrative
|
545,332
|
479,499
|
1,071,546
|
6,383,182
|
|||||||||
|
Depreciation
and amortization
|
213,009
|
372,957
|
722,817
|
2,750,701
|
|||||||||
|
Total
operating expenses
|
2,810,046
|
2,567,575
|
5,224,525
|
23,418,866
|
|||||||||
|
Other
(income) and expenses:
|
|||||||||||||
|
Interest
income
|
(14,740
|
)
|
(13,584
|
)
|
(27,142
|
)
|
(491,607
|
)
|
|||||
|
Interest
expense
|
268,555
|
60,482
|
2,334,991
|
||||||||||
|
Loss
on extinguishment of debt
|
350,450
|
||||||||||||
|
253,815
|
(13,584
|
)
|
33,340
|
2,193,834
|
|||||||||
|
Net
loss
|
(3,063,861
|
)
|
(2,553,991
|
)
|
(5,257,865
|
)
|
(25,612,700
|
)
|
|||||
|
|
|||||||||||||
|
Dividend
related to Series A , Series B
|
|||||||||||||
|
and
Series C Preferred stock
|
(717,027
|
)
|
(718,696
|
)
|
(1,437,154
|
)
|
(4,483,971
|
)
|
|||||
|
Net
loss attributable to common stockholders
|
$
|
(3,780,888
|
)
|
$
|
(3,272,687
|
)
|
$
|
(6,695,019
|
)
|
$
|
(30,096,671
|
)
|
|
The
notes to financial statements are made a part hereof.
F-47
|
VIVOQUEST,
INC.
|
|||||||||||||||||||||
|
(A
DEVELOPMENT STAGE ENTERPRISE)
|
|||||||||||||||||||||
|
FOR
THE PERIOD FROM SEPTEMBER 29, 1998 (INCEPTION) TO DECEMBER 31,
2004,
INCLUDING
|
|||||||||||||||||||||
|
THE
YEARS ENDED DECEMBER 31, 1999, 2000, 2001, 2002, 2003 and 2004
and
the
|
|||||||||||||||||||||
|
SIX
MONTHS ENDED JUNE 30, 2005
|
|
Stockholders'
Deficiency
|
||||||||||||||||||||||||||||||||||
|
Redeemable
Preferred Stock
|
Additional
|
Stock
|
||||||||||||||||||||||||||||||||
|
Series
A
|
Series
B
|
Common
Stock
|
Paid-in
|
Unearned
|
Subscriptions
|
Accumulated
|
||||||||||||||||||||||||||||
|
Shares
|
Amount
|
Shares
|
Amount
|
Shares
|
Amount
|
Capital
|
Compensation
|
Receivable
|
Deficit
|
Total
|
||||||||||||||||||||||||
|
Sale
of Common Stock for cash ($0.025 per share)
|
750,120
|
$
|
7,501
|
$
|
11,252
|
$
|
(825
|
)
|
$
|
17,928
|
||||||||||||||||||||||||
|
Sale
of Series A Convertible Preferred Stock ($1.00 per share, net
of issuance
costs of $2,195)
|
235,572
|
$
|
235,572
|
(2,195
|
)
|
(2,195
|
)
|
|||||||||||||||||||||||||||
|
Accretion
to redemption value of Series A Convertible
|
||||||||||||||||||||||||||||||||||
|
Preferred
Stock
|
4,473
|
(4,473
|
)
|
(4,473
|
)
|
|||||||||||||||||||||||||||||
|
Net
loss for the period September 29, 1998 (inception) to December
31,
1998
|
$
|
(96,405
|
)
|
(96,405
|
)
|
|||||||||||||||||||||||||||||
|
Balance
at December 31, 1998
|
235,572
|
240,045
|
750,120
|
7,501
|
4,584
|
(825
|
)
|
(96,405
|
)
|
(85,145
|
)
|
|||||||||||||||||||||||
|
Issuance
of Common Stock to executive consultants ($0.025 per
share)
|
200,000
|
2,000
|
3,000
|
5,000
|
||||||||||||||||||||||||||||||
|
Sale
of Common Stock for cash and notes ($0.025 per
share)
|
1,979,970
|
19,800
|
29,699
|
(35,071
|
)
|
14,428
|
||||||||||||||||||||||||||||
|
Sales
of Series A Convertible Preferred Stock ($1.00 per share, net
of issuance
costs of $12,824)
|
235,573
|
235,573
|
(12,824
|
)
|
(12,824
|
)
|
||||||||||||||||||||||||||||
|
Sale
of Series B convertible Preferred Stock ($2.625 per share, net
of issuance
costs of $ 73,119)
|
1,904,762
|
$
|
5,000,000
|
(73,119
|
)
|
(73,119
|
)
|
|||||||||||||||||||||||||||
|
Sale
of warrants to purchase Common Stock at $0.13125 per share to
Series B
Preferred stockholders ($0.01 per share)
|
2,000
|
2,000
|
||||||||||||||||||||||||||||||||
|
Issuance
of Common Stock to executive consultants ($0.13125 per
share)
|
400,000
|
4,000
|
48,500
|
$
|
(52,500
|
)
|
|
|||||||||||||||||||||||||||
|
Amortization
of unearned compensation
|
26,250
|
26,250
|
||||||||||||||||||||||||||||||||
|
Accretion
to redemption value of Series A Convertible Preferred
Stock
|
27,423
|
(1,840
|
)
|
(25,583
|
)
|
(27,423
|
)
|
|||||||||||||||||||||||||||
|
Accretion
to redemption value of Series B Convertible Preferred
Stock
|
80,164
|
(80,164
|
)
|
(80,164
|
)
|
|||||||||||||||||||||||||||||
|
Repayment
of Stock Subscriptions Receivable
|
825
|
825
|
||||||||||||||||||||||||||||||||
|
Net
loss for the year ended December 31, 1999
|
(679,166
|
)
|
(679,166
|
)
|
||||||||||||||||||||||||||||||
|
Balance
at December 31, 1999
|
471,145
|
503,041
|
1,904,762
|
5,080,164
|
3,330,090
|
33,301
|
—
|
(26,250
|
)
|
(35,071
|
)
|
(881,318
|
)
|
(909,338
|
)
|
|||||||||||||||||||
|
Sale
of Common Stock for cash and notes ($0.13125 per
share)
|
1,010,000
|
10,100
|
122,463
|
(93,984
|
)
|
38,579
|
||||||||||||||||||||||||||||
|
Amortization
of unearned compensation
|
26,250
|
26,250
|
||||||||||||||||||||||||||||||||
|
Accretion
to redemption value of Series A Convertible Preferred
Stock
|
32,980
|
(32,980
|
)
|
(32,980
|
)
|
|||||||||||||||||||||||||||||
|
Accretion
to redemption value of Series B Convertible Preferred
Stock
|
350,000
|
(55,599
|
)
|
(294,401
|
)
|
(350,000
|
)
|
|||||||||||||||||||||||||||
|
Repurchase
of 200,000 shares ($0.13125 per share)
|
(200,000
|
)
|
(2,000
|
)
|
(24,250
|
)
|
(26,250
|
)
|
||||||||||||||||||||||||||
|
Repayment
of Stock Subscription Receivable
|
4,881
|
4,881
|
||||||||||||||||||||||||||||||||
|
Purchase
of unvested Common shares from a terminated employee ($0.13125
per
share)
|
(111,000
|
)
|
(1,110
|
)
|
(9,634
|
)
|
10,744
|
|||||||||||||||||||||||||||
|
Net
loss for the year ended December 31, 2000
|
(1,207,635
|
)
|
(1,207,635
|
)
|
||||||||||||||||||||||||||||||
|
Balance
at December 31, 2000 (carry forward)
|
471,145
|
536,021
|
1,904,762
|
5,430,164
|
4,029,090
|
40,291
|
—
|
—
|
(113,430
|
)
|
(2,383,354
|
)
|
(2,456,493
|
)
|
||||||||||||||||||||
|
Securities
issued in connection with services are valued based upon the
estimate of
fair value of the securities issued as determined by an independent
third
party appraisal or as determined by the Board of
Directors.
|
||||||||||||||||||||||||||||||||||
The
notes to financial statements are made a part hereof.
F-48
|
VIVOQUEST,
INC.
|
|||||||||||||||||||||||
|
(A
DEVELOPMENT STAGE ENTERPRISE)
|
|||||||||||||||||||||||
|
STATEMENT
OF REDEEMABLE PREFERRED STOCK AND STOCKHOLDERS'
DEFICIENCY
|
|||||||||||||||||||||||
|
FOR
THE PERIOD FROM SEPTEMBER 29, 1998 (INCEPTION) TO DECEMBER 31,
2004,
INCLUDING
|
|||||||||||||||||||||||
|
THE
YEARS ENDED DECEMBER 31, 1999, 2000, 2001, 2002, 2003 AND 2004
AND
THE
|
|||||||||||||||||||||||
|
SIX
MONTHS ENDED JUNE 30, 2005
(CONTINUED)
|
|
Stockholders'
Deficiency
|
|||||||||||||||||||||||||||||||||||||
|
Redeemable
Preferred Stock
|
Additional
|
Stock
|
|||||||||||||||||||||||||||||||||||
|
Series
A
|
Series
B
|
Series
C
|
Common
Stock
|
Paid-in
|
Subscriptions
|
Accumulated
|
|||||||||||||||||||||||||||||||
|
Shares
|
Amount
|
Shares
|
Amount
|
Shares
|
Amount
|
Shares
|
Amount
|
Capital
|
Receivable
|
Deficit
|
Total
|
||||||||||||||||||||||||||
|
Balance
at December 31, 2000 (Brought forward)
|
471,145
|
$
|
536,021
|
1,904,762
|
$
|
5,430,164
|
4,029,090
|
$
|
40,291
|
$
|
-
|
$
|
(113,430
|
)
|
$
|
(2,383,354
|
)
|
$
|
(2,456,493
|
)
|
|||||||||||||||||
|
Sale
of Common Stock for cash and notes ($0.13125 per
share)
|
548,000
|
5,480
|
66,445
|
(71,925
|
)
|
|
|||||||||||||||||||||||||||||||
|
Accretion
to redemption value of Series A Convertible Preferred
Stock
|
32,980
|
(32,980
|
)
|
(32,980
|
)
|
||||||||||||||||||||||||||||||||
|
Accretion
to redemption value of Series B Convertible Preferred
Stock
|
350,000
|
(350,000
|
)
|
(350,000
|
)
|
||||||||||||||||||||||||||||||||
|
Purchase
of unvested Common shares from terminated employees ($0.13125
per
share)
|
(444,000
|
)
|
(4,440
|
)
|
(53,835
|
)
|
56,475
|
(1,800
|
)
|
||||||||||||||||||||||||||||
|
Repayment
of Stock Subscription Receivable
|
16,356
|
16,356
|
|||||||||||||||||||||||||||||||||||
|
Issuance
of 659,421 warrants ($1.3125 per share) in connection with Bridge
Notes
(see Note 8b)
|
1,177,366
|
1,177,366
|
|||||||||||||||||||||||||||||||||||
|
Net
loss for the year ended December 31, 2001
|
(4,382,517
|
)
|
(4,382,517
|
)
|
|||||||||||||||||||||||||||||||||
|
Balance
at December 31, 2001
|
471,145
|
569,001
|
1,904,762
|
5,780,164
|
4,133,090
|
41,331
|
806,996
|
(112,524
|
)
|
(6,765,871
|
)
|
(6,030,068
|
)
|
||||||||||||||||||||||||
|
Sale
of Common Stock for cash and notes ($0.13125 per
share)
|
100,000
|
1,000
|
12,125
|
(13,125
|
)
|
|
|||||||||||||||||||||||||||||||
|
Accretion
to redemption value of Series A Convertible Preferred
Stock
|
32,980
|
(32,980
|
)
|
(32,980
|
)
|
||||||||||||||||||||||||||||||||
|
Accretion
to redemption value of Series B Convertible Preferred
Stock
|
350,000
|
(350,000
|
)
|
(350,000
|
)
|
||||||||||||||||||||||||||||||||
|
Issuance
of stock option granted in consideration for consulting
services
|
1,956
|
1,956
|
|||||||||||||||||||||||||||||||||||
|
Repayment
of Stock Subscription Receivable
|
9,250
|
9,250
|
|||||||||||||||||||||||||||||||||||
|
Issuance
of 605,714 warrants ($1.3125 per share) in connection with Bridge
Notes
(see Note 8b)
|
475,987
|
475,987
|
|||||||||||||||||||||||||||||||||||
|
Net
loss for the year ended December 31, 2002
|
(5,923,000
|
)
|
(5,923,000
|
)
|
|||||||||||||||||||||||||||||||||
|
Balance
at December 31, 2002
|
471,145
|
601,981
|
1,904,762
|
6,130,164
|
4,233,090
|
42,331
|
914,084
|
(116,399
|
)
|
(12,688,871
|
)
|
(11,848,855
|
)
|
||||||||||||||||||||||||
|
Sale
of Common Stock for cash and notes ($0.13125 per
share)
|
1,523,159
|
15,232
|
76,158
|
91,390
|
|||||||||||||||||||||||||||||||||
|
Sale
of Series C Convertible Preferred Stock for notes ($.01 per share,
net of
issuance costs of $58,836)
|
28,224,878
|
$
|
15,063,053
|
(61,140
|
)
|
(61,140
|
)
|
||||||||||||||||||||||||||||||
|
Accretion
to redemption value of Series A Convertible Preferred
Stock
|
32,980
|
(32,980
|
)
|
(32,980
|
)
|
||||||||||||||||||||||||||||||||
|
Accretion
to redemption value of Series B Convertible Preferred
Stock
|
350,000
|
(350,000
|
)
|
(350,000
|
)
|
||||||||||||||||||||||||||||||||
|
Accretion
to redemption value of Series C Convertible Preferred
Stock
|
685,810
|
(553,102
|
)
|
(132,708
|
)
|
(685,810
|
)
|
||||||||||||||||||||||||||||||
|
Issuance
of stock option granted in consideration for consulting
services
|
6,980
|
6,980
|
|||||||||||||||||||||||||||||||||||
|
Net
loss for the year ended December 31, 2003
|
(5,002,251
|
)
|
(5,002,251
|
)
|
|||||||||||||||||||||||||||||||||
|
Balance
at December 31, 2003 (carry forward)
|
471,145
|
634,961
|
1,904,762
|
6,480,164
|
28,224,878
|
15,748,863
|
5,756,249
|
57,563
|
—
|
(116,399
|
)
|
(17,823,830
|
)
|
(17,882,666
|
)
|
||||||||||||||||||||||
Securities
issued in connection with services are valued based upon the estimate
of fair
value of the securities issued as determined by an independent third
party
appraisal or as determined by the Board of Directors.
The
notes
to financial statements are made a part hereof.
F-49
|
VIVOQUEST,
INC.
|
|||||||||||||||||||||||
|
(A
DEVELOPMENT STAGE ENTERPRISE)
|
|||||||||||||||||||||||
|
STATEMENT
OF REDEEMABLE PREFERRED STOCK AND STOCKHOLDERS'
DEFICIENCY
|
|||||||||||||||||||||||
|
FOR
THE PERIOD FROM SEPTEMBER 29, 1998 (INCEPTION) TO DECEMBER
31, 2004,
INCLUDING
|
|||||||||||||||||||||||
|
THE
YEARS ENDED DECEMBER 31, 1999, 2000, 2001, 2002, 2003 AND 2004
AND
THE
|
|||||||||||||||||||||||
|
SIX
MONTHS ENDED JUNE 30, 2005
(CONTINUED)
|
|
Stockholders'
Deficiency
|
|||||||||||||||||||||||||||||||||||||
|
Redeemable
Preferred Stock
|
Additional
|
Stock
|
|||||||||||||||||||||||||||||||||||
|
Series
A
|
Series
B
|
Series
C
|
Common
Stock
|
Paid-in
|
Subscriptions
|
Accumulated
|
|||||||||||||||||||||||||||||||
|
Shares
|
Amount
|
Shares
|
Amount
|
Shares
|
Amount
|
Shares
|
Amount
|
Capital
|
Receivable
|
Deficit
|
Total
|
||||||||||||||||||||||||||
|
Balance
at December 31, 2003 (brought forward)
|
471,145
|
634,961
|
1,904,762
|
6,480,164
|
28,224,878
|
15,748,863
|
5,756,249
|
57,563
|
—
|
(116,399
|
)
|
(17,823,830
|
)
|
(17,882,666
|
)
|
||||||||||||||||||||||
|
Accretion
to redemption value of Series A Convertible Preferred
Stock
|
32,981
|
(32,981
|
)
|
(32,981
|
)
|
||||||||||||||||||||||||||||||||
|
Accretion
to redemption value of Series B Convertible Preferred
Stock
|
350,000
|
(350,000
|
)
|
(350,000
|
)
|
||||||||||||||||||||||||||||||||
|
Accretion
to redemption value of Series C Convertible Preferred
Stock
|
1,054,415
|
(1,054,415
|
)
|
(1,054,415
|
)
|
||||||||||||||||||||||||||||||||
|
Net
loss for the year ended December 31, 2004
|
(5,257,865
|
)
|
(5,257,865
|
)
|
|||||||||||||||||||||||||||||||||
|
Balance
at December 31, 2004
|
471,145
|
667,942
|
1,904,762
|
6,830,164
|
28,224,878
|
16,803,278
|
5,756,249
|
57,563
|
(1,437,396
|
)
|
(116,399
|
)
|
(23,081,695
|
)
|
(24,577,927
|
)
|
|||||||||||||||||||||
|
(Unaudited):
|
|||||||||||||||||||||||||||||||||||||
|
Exercise
of stock option for common stock
|
13,750
|
137
|
1,667
|
(979
|
)
|
825
|
|||||||||||||||||||||||||||||||
|
Accretion
to redemption value of Series A Convertible Preferred
Stock
|
16,488
|
(16,488
|
)
|
(16,488
|
)
|
||||||||||||||||||||||||||||||||
|
Accretion
to redemption value of Series B Convertible Preferred
Stock
|
175,002
|
(175,002
|
)
|
(175,002
|
)
|
||||||||||||||||||||||||||||||||
|
Accretion
to redemption value of Series C Convertible Preferred
Stock
|
527,204
|
(527,204
|
)
|
(527,204
|
)
|
||||||||||||||||||||||||||||||||
|
Net
loss for the six months ended June 30, 2005
|
(3,063,861
|
)
|
(3,063,861
|
)
|
|||||||||||||||||||||||||||||||||
|
Balance
at June 30, 2005
|
471,145
|
$
|
684,430
|
1,904,762
|
$
|
7,005,166
|
28,224,878
|
$
|
17,330,482
|
5,769,999
|
$
|
57,700
|
$
|
(2,154,423
|
)
|
$
|
(117,378
|
)
|
$
|
(26,145,556
|
)
|
$
|
(28,359,657
|
)
|
|||||||||||||
|
Securities
issued in connection with services are valued based upon the
estimate of
fair value of the securities issued as determined by an independent
third
party appraisal or as determined by the Board of
Directors.
|
|||||||||||||||||||||||||||||||||||||
The
notes to financial statements are made a part hereof.
|
VIVOQUEST,
INC.
|
|||||||
|
(A
DEVELOPMENT STAGE ENTERPRISE)
|
|||||||
|
Cumulatve
from
|
|||||||||||||
|
Six
Months
|
September
29, 1998
|
||||||||||||
|
Ended
|
Year
Ended
|
(inception)
to
|
|||||||||||
|
June
30,
|
December
31,
|
June
30,
|
|||||||||||
|
2005
|
2004
|
2004
|
2005
|
||||||||||
|
(unaudited)
|
(unaudited)
|
(unaudited)
|
|||||||||||
|
Cash
flows from operating activities:
|
|||||||||||||
|
Net
loss
|
$
|
(3,063,861
|
)
|
$
|
(2,553,991
|
)
|
$
|
(5,257,865
|
)
|
$
|
(25,612,700
|
)
|
|
|
Adjustments
to reconcile net loss to
|
|||||||||||||
|
net
cash used in operating activities:
|
|||||||||||||
|
Depreciation
and amortization
|
213,009
|
372,957
|
722,817
|
2,750,701
|
|||||||||
|
Amortization
of discount on notes payable
|
1,302,903
|
||||||||||||
|
Loss
on extinguishment of debt
|
350,450
|
||||||||||||
|
Stock
issued for accrued interest on notes
|
155,896
|
||||||||||||
|
Stock
and stock options issued in consideration
|
|||||||||||||
|
for
services rendered
|
157,826
|
||||||||||||
|
Changes
in assets and liabilities:
|
|||||||||||||
|
Decrease
(increase) in prepaid expenses, other
|
|||||||||||||
|
current
assets and other assets
|
(18,857
|
)
|
135,286
|
304,754
|
(162,596
|
)
|
|||||||
|
(Decrease)
increase in accounts payable
|
|||||||||||||
|
and
accrued expenses
|
435,310
|
12,587
|
11,800
|
1,180,250
|
|||||||||
|
Net
cash used for operating activities
|
(2,434,399
|
)
|
(2,033,161
|
)
|
(4,218,494
|
)
|
(19,877,270
|
)
|
|||||
|
Cash
flows from investing activities:
|
|||||||||||||
|
Capital
expenditures
|
(1,707
|
)
|
(131,670
|
)
|
(141,149
|
)
|
(3,331,902
|
)
|
|||||
|
Cash
flows from financing activities:
|
|||||||||||||
|
Refund
of security deposits
|
30,000
|
30,000
|
|||||||||||
|
Sale
of common stock
|
1,804
|
104,050
|
|||||||||||
|
Stock
subscriptions receivable
|
(979
|
)
|
(979
|
)
|
|||||||||
|
Repurchase
of common stock
|
(28,050
|
)
|
|||||||||||
|
Proceeds
from sale of Series A preferred stock
|
471,145
|
||||||||||||
|
Proceeds
from sale of Series B preferred stock
|
5,000,000
|
||||||||||||
|
Proceeds
from sale of Series C preferred stock
|
4,000,000
|
||||||||||||
|
Proceeds
from sale of Warrants
|
1,655,353
|
||||||||||||
|
Costs
associated with issuance of preferred stock
|
(149,278
|
)
|
|||||||||||
|
Accured
interest on notes payable
|
12,891,290
|
||||||||||||
|
Proceeds
from notes payable
|
2,100,000
|
|
2,084,642
|
||||||||||
|
Net
cash provided by financing activities
|
2,130,825
|
2,084,642
|
23,973,531
|
||||||||||
|
NET
INCREASE (DECREASE) IN CASH
|
|||||||||||||
|
AND
CASH EQUIVALENTS
|
(305,281
|
)
|
(2,164,831
|
)
|
(2,275,001
|
)
|
764,359
|
||||||
|
Cash
and cash equivalents at beginning of period
|
1,069,640
|
3,344,641
|
3,344,641
|
||||||||||
|
Cash
and cash equivalents at end of period
|
$
|
764,359
|
$
|
1,179,810
|
$
|
1,069,640
|
$
|
764,359
|
|||||
|
Supplemental
disclosure of noncash investing
|
|||||||||||||
|
and
financing activities:
|
|||||||||||||
|
Accretion
to redemption value of Series A
|
|||||||||||||
|
Preferred
stock
|
$
|
16,488
|
$
|
16,490
|
$
|
32,981
|
$
|
180,304
|
|||||
|
Accretion
to redemption value of Series B
|
|||||||||||||
|
Preferred
stock
|
175,002
|
174,999
|
350,000
|
1,655,166
|
|||||||||
|
Accretion
to redemption value of Series C
|
|||||||||||||
|
Preferred
stock
|
527,204
|
527,207
|
1,054,415
|
2,267,429
|
|||||||||
|
Series
C Preferred stock issued for notes
|
217,608
|
||||||||||||
|
payable
and accrued interest
|
|||||||||||||
|
Discount
on notes payable
|
1,653,353
|
||||||||||||
The
notes to financial statements are made a part hereof.
F-51
VIVOQUEST,
INC.
(A
DEVELOPMENT STAGE ENTERPRISE)
(INFORMATION
WITH RESPECT TO THE SIX MONTH PERIOD
ENDED
JUNE 30, 2004 AND THE PERIOD SUBSEQUENT TO
DECEMBER
31, 2004 IS UNAUDITED)
| 1. |
Organization
and Business:
|
|
VivoQuest,
Inc. (the "Company") is engaged in the discovery, development and
manufacture of therapeutic agents derived from chemical compounds
existing
in nature for the diagnosis, prophylaxis and treatment of human
diseases
and disorders. The Company was incorporated in the State of Delaware
on
September 18, 1998 and commenced operations on September 29,
1998. The Company’s operations are in the United States. As a development
stage enterprise, the Company’s primary efforts, to date, have been
devoted to raising capital, forming strategic relationships with
research
institutes, universities and commercial entities to complement
its
research and development activities, recruiting senior management
and key
scientific personnel, securing a corporate facility for research
and
administration (Valley Cottage, New York) and commencing research
operations at the corporate facility. In addition to the normal
risks
associated with a new business venture, there can be no assurance
that the
Company’s research and development will be successfully completed or that
any approved product will be commercially viable. In addition,
the Company
operates in an environment of rapid change in technology, and is
dependent
upon the services of its employees, executive officers and consultants.
The Company operates under a single
segment.
|
|
On
February 7, 2002, the Company’s Board of Directors approved a 2-for-1
stock dividend of the outstanding shares of common stock, while
maintaining the par value of common stock at $0.01. All common
share and
per share amounts included herein have been adjusted as if the
stock
dividend had occurred at inception.
|
In
September 2005, the Company sold substantially all of its assets to XTL
Biopharmaceuticals Inc., pursuant to an Asset Purchase Agreement (see Note
11).
In
September 2005, the Company also granted to XTL Biopharmaceuticals Ltd.
exclusive worldwide rights to the Company’s intellectual property and
technology, pursuant to a Licensing Agreement (see Note 11).
| 2. |
Summary
of Significant Accounting Policies:
|
Basis
of Preparation
|
The
financial statements have been prepared on a going concern basis,
which
contemplates realization of assets and liquidation of liabilities
in the
ordinary course of business. The Company has limited capital resources,
net operating losses and negative cash flows from operations since
inception and expects these conditions to continue for the foreseeable
future. In addition, it is anticipated that the Company will not
generate
revenues from product sales in the twelve months following
December 31, 2004 and in the several years following that period.
These conditions raise substantial doubt about the Company’s ability to
continue as a going concern.
|
(Continued)
F-52
VIVOQUEST,
INC.
(A
DEVELOPMENT STAGE ENTERPRISE)
NOTES
TO
FINANCIAL STATEMENTS
(INFORMATION
WITH RESPECT TO THE SIX MONTH PERIOD
ENDED
JUNE 30, 2004 AND THE PERIOD SUBSEQUENT TO
DECEMBER
31, 2004 IS UNAUDITED)
| 2. |
Summary
of Significant Accounting Policies (Continued):
|
|
Basis
of Preparation (Continued)
|
|
As
of June 30, 2005 and December 31, 2004, the Company had approximately
$760,000, and $1,069,000 in cash and cash equivalents, respectively.
During 2001 and 2002, the Company issued approximately $10.4 million
in
convertible term notes (“Bridge Notes”) (see Note 8b), the principal and
accrued interest on which were converted to shares of the Company’s Series
C Preferred Stock in March 2003. The funds raised from the Bridge
Notes
were used to pay for rent, leasehold improvements and equipment
necessary
to set up laboratory facilities as well as salaries and other operating
expenses. During April 2003 and September 2003 the Company raised
an
additional $4 million through the sale of Series C Preferred Stock.
The
Company will be required to raise additional funds to meet other
planned
obligations in the future and has sought to raise such amounts
through the
private sale of its equity securities. The Company may also seek
to raise
capital through collaborative arrangements with corporate sources
or other
sources of financing. There can be no assurance that such additional
financing, if at all available, can be obtained on terms reasonable
to the
Company. In the event that sufficient funds are not available,
the Company
will need to postpone, scale back or discontinue future operations.
Continuance of the Company as a going concern is dependent upon,
among
other things, the Company’s ability to obtain adequate long-term
financing, the success of its research and development program
and its
attainment of profitable operations. The financial statements do
not
include any adjustments that might result from the outcome of this
uncertainty.
|
Cash
and Cash Equivalents
|
The
Company considers all highly liquid investments which have maturities
of
three months or less, when acquired, to be cash equivalents. The
carrying
amount reported in the balance sheet for cash and cash equivalents
approximates its fair value. Cash and cash equivalents subject
the Company
to concentrations of credit risk. At June 30, 2005 and December 31,
2004, the Company held approximately $760,000 and $1,069,000 respectively,
in a single commercial bank.
|
Property,
Plant and Equipment
Furniture
and lab equipment and computers are stated at cost and are depreciated on
a
straight-line basis over their estimated useful lives. Leasehold improvements
are stated at cost and are amortized on a straight-line basis over the life
of
the lease or of the improvement, whichever is shorter.
(Continued)
F-53
VIVOQUEST,
INC.
(A
DEVELOPMENT STAGE ENTERPRISE)
NOTES
TO
FINANCIAL STATEMENTS
(INFORMATION
WITH RESPECT TO THE SIX MONTH PERIOD
ENDED
JUNE 30, 2004 AND THE PERIOD SUBSEQUENT TO
DECEMBER
31, 2004 IS UNAUDITED)
| 2. |
Summary
of Significant Accounting Policies (Continued):
|
Property,
Plant and Equipment (Continued)
Expenditures
for maintenance and repairs which do not materially extend the useful lives
of
the assets are charged to expense as incurred. The cost and accumulated
depreciation of assets retired or sold are removed from the respective accounts
and any gain or loss is recognized in operations. The estimated useful lives
of
fixed assets are as follows:
|
Computer
and telephone equipment
|
3
years
|
|||
|
Furniture
and lab equipment
|
5
years
|
|||
|
Leasehold
improvements
|
Life
of lease
|
Revenue
Recognition
Interest
income is recognized as earned.
Research
and Development
Research
and development costs are charged to expense as incurred.
Patents
As
a
result of research and development efforts conducted by the Company, it has
applied, or is applying for a number of patents to protect proprietary
inventions. All costs associated with patents are expensed as
incurred.
Concentration
of Credit Risk
|
Financial
instruments which potentially subject the Company to concentrations
of
credit risk consist of cash and cash
equivalents.
|
(Continued)
F-54
VIVOQUEST,
INC.
(A
DEVELOPMENT STAGE ENTERPRISE)
NOTES
TO
FINANCIAL STATEMENTS
(INFORMATION
WITH RESPECT TO THE SIX MONTH PERIOD
ENDED
JUNE 30, 2004 AND THE PERIOD SUBSEQUENT TO
DECEMBER
31, 2004 IS UNAUDITED)
| 2. |
Summary
of Significant Accounting Policies (Continued):
|
Income
Taxes
|
The
Company accounts for income taxes in accordance with the provisions
of
Statement of Financial Accounting Standards No. 109, "Accounting
for
Income Taxes" ("SFAS No. 109"). SFAS No. 109 requires that the
Company
recognize deferred tax liabilities and assets for the expected
future tax
consequences of events that have been included in the financial
statements
or tax returns. Under this method, deferred tax liabilities and
assets are
determined on the basis of the difference between the tax basis
of assets
and liabilities and their respective financial reporting amounts
("temporary differences") at enacted tax rates in effect for the
years in
which the temporary differences are expected to
reverse.
|
Use
of Estimates
|
The
preparation of financial statements in conformity with generally
accepted
accounting principles requires management to make estimates and
assumptions that affect the amounts reported in the financial statements
and accompanying notes. Significant estimates include useful lives
of
fixed assets and valuation of common stock and stock options (see
below).
Actual results could differ from those
estimates.
|
Stock-Based
Compensation
|
The
accompanying financial position and results of operations of the
Company
have been prepared in accordance with APB Opinion No. 25, "Accounting
for
Stock Issued to Employees" ("APB No. 25"). Under APB No. 25, generally,
no
compensation expense is recognized in the financial statements
in
connection with the sale of common stock or awarding of stock option
grants to employees provided that, as of the sale or grant date,
all terms
associated with the sale or award are fixed and the fair value
of the
Company's stock, as of the sale or grant date, is equal to or less
than
the amount an employee must pay to acquire the stock. The Company
will
recognize compensation expense in situations where the terms of
a stock
sale or an option grant are not fixed or where the fair value of
the
Company's common stock on the sale or grant date is greater than
the
amount an employee must pay to acquire the stock.
|
(Continued)
F-55
VIVOQUEST,
INC.
(A
DEVELOPMENT STAGE ENTERPRISE)
NOTES
TO
FINANCIAL STATEMENTS
(INFORMATION
WITH RESPECT TO THE SIX MONTH PERIOD
ENDED
JUNE 30, 2004 AND THE PERIOD SUBSEQUENT TO
DECEMBER
31, 2004 IS UNAUDITED)
|
2.
|
Summary
of Significant Accounting Policies (Continued):
|
Stock-Based
Compensation (Continued)
|
The
Company has stock-based incentive plans, which are described in
Note 9.
The following table illustrates the effect on the Company’s net loss
attributable to common stockholders had compensation costs for
the
incentive plans been determined in accordance with the fair value
based
method of accounting for stock-based compensation as prescribed
by
Statement of Financial Accounting Standards No. 123, Accounting
for Stock-Based Compensation
(“SFAS No. 123”) as amended by Statement of Financial Accounting Standards
No. 148 “Accounting for Stock-Based Compensation Transaction and
Disclosure, an amendment of SFAS 123”. Since option grants awarded vest
over several years and additional awards may be issued in the future,
the
pro forma results shown below are not likely to be representative
of the
effects on future years of the application of the fair value based
method.
|
|
Cumulative
from
|
|||||||||||||
|
Year
|
September
29,
|
||||||||||||
|
Six
Months Ended
|
Ended
|
1998
(Inception)
|
|||||||||||
|
June
30,
|
December
31,
|
to
June 30,
|
|||||||||||
|
2005
|
2004
|
2004
|
2005
|
||||||||||
|
Net
loss attributable to common stockholders, as reported
|
$
|
(3,780,888
|
)
|
$
|
(3,272,687
|
)
|
$
|
(6,695,019
|
)
|
$
|
(30,096,671
|
)
|
|
|
Deduct:
total stock-based employee compensation expense determined under
fair
value based method for all awards
|
(328
|
)
|
(26,572
|
)
|
(77,549
|
)
|
|||||||
|
Pro
forma net loss attributable to common stockholders
|
$
|
(3,781,216
|
)
|
$
|
(3,272,687
|
)
|
$
|
(6,721,591
|
)
|
$
|
(30,174,220
|
)
|
|
Continued)
F-56
VIVOQUEST,
INC.
(A
DEVELOPMENT STAGE ENTERPRISE)
NOTES
TO
FINANCIAL STATEMENTS
(INFORMATION
WITH RESPECT TO THE SIX MONTH PERIOD
ENDED
JUNE 30, 2004 AND THE PERIOD SUBSEQUENT TO
DECEMBER
31, 2004 IS UNAUDITED)
| 2. |
Summary
of Significant Accounting Policies (Continued):
|
Stock-Based
Compensation (Continued)
|
For
the purposes of the above pro forma calculations, the fair value
of each
option granted from the 1999 Stock Plan during the period and was
estimated on the date of grant using the Black Scholes option pricing
model. The following table summarizes the assumptions used in computing
the fair value of option grants for the periods presented
above.
|
|
Expected
volatility
|
85
|
%
|
||
|
Expected
lives
|
5
|
|||
|
Dividend
yield
|
0
|
%
|
||
|
Risk
free interest rate
|
3.18
|
%
|
|
Other
disclosures required by SFAS No. 123 have been included in Note
9.
|
|
The
fair value of options and warrants granted to nonemployees for
financing,
goods or services are included in the financial statements and
expensed
over the life of the debt, as the goods are utilized or the services
performed, respectively.
|
Comprehensive
Loss
|
Comprehensive
loss represents the change in net assets of a business enterprise
during a
period from transactions and other events and circumstances from
nonowner
sources. For all periods presented, there are no differences between
net
loss and comprehensive net loss.
|
(Continued)
F-57
VIVOQUEST,
INC.
(A
DEVELOPMENT STAGE ENTERPRISE)
NOTES
TO
FINANCIAL STATEMENTS
(INFORMATION
WITH RESPECT TO THE SIX MONTH PERIOD
ENDED
JUNE 30, 2004 AND THE PERIOD SUBSEQUENT TO
DECEMBER
31, 2004 IS UNAUDITED)
| 3. |
Property
Plant and Equipment:
|
|
Property,
plant and equipment as of June 30, 2005 and December 31, 2004 consist
of
the following:
|
|
June
30,
|
December
31,
|
||||||
|
2005
|
2004
|
||||||
|
Computer
and telephone equipment
|
$
|
237,279
|
$
|
235,572
|
|||
|
Furniture
and lab equipment
|
2,009,203
|
2,009,203
|
|||||
|
Leasehold
improvements
|
1,085,770
|
1,085,770
|
|||||
|
3,332,252
|
3,330,545
|
||||||
|
Less
accumulated depreciation and amortization
|
(2,751,051
|
)
|
(2,538,042
|
)
|
|||
|
$
|
581,201
|
$
|
792,503
|
||||
|
Depreciation
and amortization of fixed assets was approximately $213,000, $373,000,
$723,000 and $2,751,000 for the six months ended June 30, 2005,
June 30,
2004, the year ended December 31, 2004 and the cumulative period
from
September 29, 1998 (inception) to June 30, 2005,
respectively.
|
| 4. |
Accounts
Payable and Accrued Expenses:
|
|
Accounts
payable and accrued expenses as of June 30, 2005 and December 31,
2004
consist of the following:
|
|
June
30,
|
December
31,
|
||||||
|
2005
|
2004
|
||||||
|
Accounts
payable
|
$
|
75,014
|
$
|
80,822
|
|||
|
Accrued
professional fees
|
53,619
|
56,480
|
|||||
|
Accrued
interest payable
|
329,038
|
60,481
|
|||||
|
Accrued
research contract expenses
|
175,422
|
—
|
|||||
|
$
|
633,093
|
$
|
197,783
|
||||
(Continued)
F-58
VIVOQUEST,
INC.
(A
DEVELOPMENT STAGE ENTERPRISE)
NOTES
TO
FINANCIAL STATEMENTS
(INFORMATION
WITH RESPECT TO THE SIX MONTH PERIOD
ENDED
JUNE 30, 2004 AND THE PERIOD SUBSEQUENT TO
DECEMBER
31, 2004 IS UNAUDITED)
| 5. |
Convertible
Secured Promissory Note Payable:
|
|
In
September 2004, the Company entered into a convertible secured
promissory
note with UPMC Health System, a Pennsylvania non-profit corporation
(“the
Holder”). The Company can borrow up to $2,500,000 with an interest of
10%.
The note is automatically due and payable on the earlier of (a)
12 months
after the date of the note or (b) the occurrence of an event of
default as
specified in the agreement. Any unpaid portion of principal with
accrued
interest will be automatically converted into shares of the Company’s
equity securities issued and sold at the closing of a Qualified
Financing
that occurs on or prior to the maturity date. As of June 30, 2005
and
December 31, 2004, the note has an outstanding balance of approximately
$2,485,000 and $1,235,000,
respectively.
|
|
In
September 2004, the Company entered into another convertible secured
promissory note with Highmark Health Ventures Investment Fund,
L.P. (“the
Holder”). The Company can borrow up to $1,700,000 with an interest at
10%
a year. The note is automatically due and payable on the earlier
of (a) 12
months after the date of the note or (b) the occurrence of an event
of
default as specified in the agreement. Any unpaid portion of principal
with accrued interest will be automatically converted into shares
of the
Company’s equity securities issued and sold at the closing of a Qualified
Financing that occurs on or prior to the maturity date, September
16,
2005. As of June 30, 2005 and December 31, 2004, the note has an
outstanding principal balance of approximately $1,700,000 and $850,000,
respectively.
|
|
Per
the note payable agreements, if there is a change in control prior
to the
maturity date of the notes, the notes shall be payable in the amount
of
2.5 times the sum of the principal plus any accrued interest. Due
to the
Asset Purchase Agreement (see Note 11), a change in control occurred.
In
relation to a distribution of assets agreement, the note holders
agreed
that the maximum amount that the Company would be liable for the
notes
would be $7,500,000 payable upon receipt of additional monies into
the
Company in a ratio of 91.3% of all distributable
assets.
|
(Continued)
F-59
VIVOQUEST,
INC.
(A
DEVELOPMENT STAGE ENTERPRISE)
NOTES
TO
FINANCIAL STATEMENTS
(INFORMATION
WITH RESPECT TO THE SIX MONTH PERIOD
ENDED
JUNE 30, 2004 AND THE PERIOD SUBSEQUENT TO
DECEMBER
31, 2004 IS UNAUDITED)
| 6. |
Stockholders’
Equity:
|
The
Company’s Certificate of Incorporation, as amended, authorizes the Company to
issue 49,400,000
shares of common stock (the “Common Stock”), $0.01 par value.
At
June 30, 2005, the following numbers of shares of Common Stock have been
reserved: (i) 942,290 shares for issuance upon conversion of A Preferred
(see
Note 7), (ii) 6,629,190 shares for issuance upon conversion of B Preferred
(see
Note 7), (iii) 200,000 shares for issuance upon exercise of warrants sold
in
connection with B Preferred (see Note 7), (iv) 28,224,878 shares for issuance
upon conversion of C preferred (see Note 7); (v) 3,243,517 shares for issuance
upon exercise of 2001 Bridge Warrants (see Note 8), and (vi) 6,869,047 shares
issuable under the 1999 Stock Plan (see Note 9).
|
In
connection with the purchase of Common Stock, employees, consultants
and
investors issued full recourse promissory notes to the Company
for a
portion of the purchase price. The principal accrues interest at
a rate of
5.74% per annum. Principal and accrued interest is due on various
dates
between July 1, 2004 and June 30, 2007. Purchasers may prepay
principal and accrued interest without penalty. In the case of
events of
default by these individuals, as defined, the unpaid principal
and accrued
interest will become immediately due to the Company. The agreements
provide for restriction of future sale or transfer of a portion
of the
Common Stock issued to employees and consultants. Such restrictions
lapse
ratably from March 1, 2002 through November 21, 2005. Upon termination
of
employment of any consultant or employee, the Company will have
the right,
but not the obligation, to purchase remaining restricted shares
at their
then fair value. The Company recorded a receivable of $116,399
at December
31, 2004 and $117,378 at June 30, 2005 from the sale of Common
Stock
issued to employees and
consultants.
|
|
As
of April 6, 2006, the date of this report, none of the promissory
notes
have been repayed to the Company.
|
(Continued)
F-60
VIVOQUEST,
INC.
(A
DEVELOPMENT STAGE ENTERPRISE)
NOTES
TO
FINANCIAL STATEMENTS
(INFORMATION
WITH RESPECT TO THE SIX MONTH PERIOD
ENDED
JUNE 30, 2004 AND THE PERIOD SUBSEQUENT TO
DECEMBER
31, 2004 IS UNAUDITED)
| 6. |
Stockholders’
Equity (Continued):
|
|
On
September 30, 1999, the Company entered into agreements (the “Management
Agreements”) with the Company’s Chairman and Interim Chief Executive
Officer and Chief Financial Officer (the “Officers”) for services they had
performed in organizing and raising financing for the Company and
services
they will perform in the future in those same capacities. In consideration
for services rendered under the Management Agreements, the Company
issued
200,000 shares of Common Stock to each of the Officers. The fair
value of
those shares of Common Stock on the issuance date was $0.2625 per
share as
determined by an independent third party appraisal which was subsequently
revalued at $0.13125 after a 2-for-1 stock split. Accordingly,
the Company
recorded unearned compensation of $52,500 in connection with the
shares
issued to the Officers. For each of the years ended December 31,
2000 and
1999, the Company recognized compensation expense of $26,250 in
connection
with the shares issued to the Officers. The Management Agreements
terminated on March 31, 2001.
|
|
During
2003, the Company granted a total of 1,523,159 shares of common
stock to
employees and one nonemployee consultant for services rendered.
In
connection with these awards, the Company recognized $91,390 of
compensation expense, reflecting a fair value of common stock of
$0.06 on
the dates of grant as determined by the Board of Directors. During
2005,
the Company issued 13,750 shares of common stock due to an employee
exercising an option at an exercised price of $0.13125 (see Note
9).
|
There
were no shares of common stock granted to employees for services in
2004.
| 7. |
Mandatorily
Redeemable Convertible Preferred Stock and
Warrants:
|
|
The
Company’s Certificate of Incorporation, as amended, authorizes the Company
to issue 33,844,305 shares of preferred stock (the “Preferred Stock”), of
which 471,145 shares are designated as Series A Convertible Preferred
Stock $1.00 par value (the “A Preferred”), and 1,904,762 shares are
designated as Series B Convertible Preferred Stock $1.00 par value
(the “B
Preferred”), and 31,468,398 shares are designated as Series C Convertible
Preferred Stock $.01 par value (the “C
Preferred”).
|
(Continued)
F-61
VIVOQUEST,
INC.
(A
DEVELOPMENT STAGE ENTERPRISE)
NOTES
TO
FINANCIAL STATEMENTS
(INFORMATION
WITH RESPECT TO THE SIX MONTH PERIOD
ENDED
JUNE 30, 2004 AND THE PERIOD SUBSEQUENT TO
DECEMBER
31, 2004 IS UNAUDITED)
| 7. |
Mandatorily
Redeemable Convertible Preferred Stock and Warrants
(Continued):
|
|
In
September 1998 and May 1999, an investor (the “Initial Investor”)
purchased 235,572 shares and 235,573 shares, respectively, of A
Preferred
for $1.00 per share. In September and December 1999, four investors,
including the Initial Investor, purchased a total of 1,904,762
shares of B
Preferred for $2.625 per share. In the event of liquidation, dissolution
or winding up of the Company, holders of A Preferred and B Preferred
will
be entitled to be paid $1.00 and $2.625 per share, respectively,
subject
to adjustment for stock dividends, stock splits, mergers or other
recapitalization, as defined, plus all dividends accrued or declared
but
unpaid, out of the assets of the Company. The order of preference
of
payments will be to holders of B Preferred, then A Preferred and
then
Common Stock.
|
|
Each
share of A Preferred and B Preferred is convertible into the number
of
shares of Common Stock determined by dividing $1.00 by the Series
A
Conversion Price or $2.625 by the Series B Conversion Price, respectively.
The Conversion Price at which shares of Common Stock shall be delivered
upon conversion of A Preferred or B Preferred without payment of
any
additional consideration by the holder thereof shall initially
be $1.00 or
$2.625 per share of Common Stock, respectively. The Series A Conversion
Price and Series B Conversion Price are subject to adjustments
under
certain circumstances as defined, in effect at the time of the
conversion
including each time the Company sells additional shares of Common
Stock
that are not part of a stock option, stock purchase or stock bonus
plan,
at a fair market value which is below the Conversion Price in effect
at
the time of sale. The Initial Investor, the sole owner of A Preferred,
has
waived all rights to an adjustment to the Conversion Price resulting
from
issuances of Common Stock prior to October 1, 1999. Accrued but
unpaid dividends are forfeited upon conversion of A Preferred or
B
Preferred. As of June 30, 2005, the Series A Conversion Price was
$0.50
and the Series B Conversion Price was $0.75424 after the effect
of the
2-for-1 stock dividend (see Note 1) and the anti-dilution provision
resulting from issuance of C Preferred (see below). The outstanding
A
Preferred and B Preferred were convertible into 942,290 and 6,629,190
shares of Common Stock,
respectively.
|
(Continued)
F-62
VIVOQUEST,
INC.
(A
DEVELOPMENT STAGE ENTERPRISE)
NOTES
TO
FINANCIAL STATEMENTS
(INFORMATION
WITH RESPECT TO THE SIX MONTH PERIOD
ENDED
JUNE 30, 2004 AND THE PERIOD SUBSEQUENT TO
DECEMBER
31, 2004 IS UNAUDITED)
| 7. |
Mandatorily
Redeemable Convertible Preferred Stock and Warrants
(Continued):
|
|
In
March, April and September 2003, the Company authorized 25,847,050
shares
of Series C Preferred Stock with a stated value of $0.53368 per
share in
connection with a Qualified Financing. At that time, the principal
and
accrued interest on Bridge Notes issued in 2001 and 2002 (see Note
8b),
totaling approximately $11.1 million, were converted into 20,729,747
shares of C Preferred at a conversion price of $0.53368 and an
additional
1,873,782 shares of C Preferred were purchased for $1.0 million
by the
initial Investor. In September 2003, the Company authorized an
additional
5,621,348 shares of Series C Preferred Stock with a stated value
of
$.053368 per share, which were purchased by two investors. The
C Preferred
has the same terms as B Preferred as to liquidation, conversion,
redemption, dividends and voting except that the stated value and
redemption value for C Preferred are $0.53368 per share and the
liquidation value for C Preferred is $0.80052 per share. Upon events
of
liquidation and payment of dividends, the preference of payments
is to
holders of C Preferred and B Preferred, before holders of A Preferred
and
Common Stock.
|
|
As
a result of the anti-dilution provisions associated with the B
Preferred,
upon issuance of the shares of C Preferred in March 2003, the Conversion
Price of B Preferred changed from $1.3125 to $0.75424 and the 3,804,524
shares of B Preferred are convertible into 6,629,190
shares.
|
|
Shares
of A Preferred, B Preferred and C Preferred will automatically
convert
into shares of Common Stock based upon the Series A Conversion
Price,
Series B Conversion Price and Series C Conversion Price in effect
at the
time upon (i) the closing of an initial public offering of the
Company’s
Common Stock, within defined terms or (ii) written election of
the holders
of at least two-thirds of A Preferred, B Preferred or C
Preferred.
|
|
Holders
of A Preferred, B Preferred and C Preferred have the number of
votes equal
to the number of shares of Common Stock into which the shares of
Preferred
Stock held by that shareholder would be converted at the date on
which the
vote is held. As of December 31, 2004 and June 30, 2005, such votes
total
35,796,358.
|
(Continued)
F-63
VIVOQUEST,
INC.
(A
DEVELOPMENT STAGE ENTERPRISE)
NOTES
TO
FINANCIAL STATEMENTS
(INFORMATION
WITH RESPECT TO THE SIX MONTH PERIOD
ENDED
JUNE 30, 2004 AND THE PERIOD SUBSEQUENT TO
DECEMBER
31, 2004 IS UNAUDITED)
| 7. |
Mandatorily
Redeemable Convertible Preferred Stock and Warrants
(Continued):
|
|
Dividends
may be declared and paid on Common Stock, as determined by the
Company’s
Board of Directors, provided (i) that all dividends, accrued or
declared,
to holders of Preferred Stock have previously been paid and (ii)
that at
the same time, the Company declares and pays a dividend to the
holders of
Preferred Stock equal to that which would be payable to them if
their
Preferred Stock had been converted into Common Stock on the date
of
determination of holders of Common Stock to receive such
dividend.
|
|
Dividends
may be declared and paid on Preferred Stock, as determined by the
Company’s Board of Directors provided (i) that no dividends will be paid
to holders of A Preferred until all dividends, accrued or declared,
to
holders of B Preferred and C Preferred have previously been paid
and (ii)
that at the time dividends are declared and paid to holders of
A
Preferred, the Company declares and pays a dividend to the holders
of B
Preferred and C Preferred equal to that which would be payable
to them if
their B Preferred and C Preferred had been converted into Common
Stock.
|
|
A
,
B and C Preferred shareholders are entitled to receive dividends
at the
rate of 7.0% per share per annum of the stated value, $1.00, $2.625
and
$0.53368, respectively, subject to adjustment for stock dividends,
stock
splits, mergers or recapitalizations, as defined. As of December
31, 2004
and June 30, 2005, the stated value was $1.00 per share of A Preferred,
2.625 per share of B Preferred and $0.53368 per share of C Preferred.
Dividends are cumulative and accrue from the date of issue, whether
or not
earned or declared.
|
|
At
the written election of any holder of Preferred Stock made within
30 days
of each of March 20, 2008, 2009 and 2010, the Company will redeem,
within
60 days after each March 20, from such holder up to one-third of
the
shares of Preferred Stock held by such holder, at a redemption
price per
share of $1.00, plus dividends accrued or declared but unpaid,
for A
Preferred and $2.625, plus dividends accrued or declared but unpaid,
for B
Preferred and $0.53368, plus dividends accrued or declared but
unpaid for
C Preferred (the “Redemption Price”). The Redemption Price is subject to
adjustment for stock dividends, stock splits, mergers or
recapitalizations, as defined.
|
(Continued)
F-64
VIVOQUEST,
INC.
(A
DEVELOPMENT STAGE ENTERPRISE)
NOTES
TO
FINANCIAL STATEMENTS
(INFORMATION
WITH RESPECT TO THE SIX MONTH PERIOD
ENDED
JUNE 30, 2004 AND THE PERIOD SUBSEQUENT TO
DECEMBER
31, 2004 IS UNAUDITED)
| 7. |
Mandatorily
Redeemable Convertible Preferred Stock and Warrants
(Continued):
|
|
Mandatorily
redeemable preferred stock is recorded at redemption value, which
equals
issuance price plus accretion of dividends accrued or declared
but unpaid.
At June 30, 2005 and December 31, 2004 such accretion amounted
to $213,286
and $196,796 for A Preferred and $2,005,164 and $1,830,164 for
B Preferred
and $2,267,431 and $1,740,225 for C Preferred,
respectively.
|
|
In
connection with the sale of B Preferred in September 1999, the
Company
sold warrants to individuals who were employees of the investors
in B
Preferred. Each warrant entitles the holder to purchase a defined
number
of shares of Common Stock (“Warrant Shares”) (aggregating 200,000 shares
for all warrant holders) at an exercise price of $0.13125 per share.
Each
warrant holder had paid $0.01 per Warrant Share. The exercise price
per
share and number of Warrant Shares are subject to adjustment, as
defined.
The warrants expire in September 2009. At June 30, 2005 and
December 31, 2004, none of the warrants had been
exercised.
|
| 8. |
Commitments
and Contingencies:
|
| (a) |
Operating
Leases
|
|
In
September, 1998 and July 1999 the Company entered into a series
of
agreements with the Initial Investor for the assignment of noncancelable
lease agreements for office space in New York City into which the
Initial
Investor had entered (the “Leases”). The Leases have terms of three to six
months, are automatically renewable at the option of the assignee
and
provide for escalation of the minimum rent at each anniversary
for each
lease. Rental expense in connection with the Leases amounted to
approximately $18,000 for each of the six month periods ended June
30,
2005 and 2004, $36,000 for the year ended December 31, 2004 and
$310,000
the period from September 29, 1998 (inception) to June 30,
2005.
|
(Continued)
F-65
VIVOQUEST,
INC.
(A
DEVELOPMENT STAGE ENTERPRISE)
NOTES
TO
FINANCIAL STATEMENTS
(INFORMATION
WITH RESPECT TO THE SIX MONTH PERIOD
ENDED
JUNE 30, 2004 AND THE PERIOD SUBSEQUENT TO
DECEMBER
31, 2004 IS UNAUDITED)
| 8. |
Commitments
and Contingencies (Continued):
|
| (a) |
Operating
Leases (Continued)
|
|
In
February 2001, the Company entered into a four year sublease agreement
for
laboratory and office facilities in Valley Cottage, New York (the
“Valley
Cottage Sublease”). As part of the Valley Cottage Sublease, the Company
made a $2.7 million payment, which included a $1,069,200 prepayment
of
base rent through November 30, 2004, $1,071,830 for the purchase
of
leasehold improvements and $558,970 for equipment and furniture.
Rent
expense for the Valley Cottage Sublease amounted to approximately
$146,000, $146,000, $304,000 and $1,253,000 for the six months
ended June
30, 2005 and 2004, year ended December 31, 2004, and the period
from
September 29, 1998 (inception) to June 30, 2005,
respectively.
|
|
In
addition to the base rent, the Company is also required to pay
its pro
rata share of real estate taxes, insurance premiums and common
area costs
(“Additional Rental Charges”). Additional rent charges for the six months
ended June 30, 2005 and 2004, year ended December 31, 2004, and
the period
from September 29, 1998 (inception) to June 30, 2005 are $43,800,
$43,800,
$76,000 and $350,000, respectively. In November 2002, the Company
received
a rebate from the landlord of approximately $54,000 representing
an
adjustment of the additional rent for the period from April 2001
through
November 2002. Such amount was recorded as a reduction of the 2002
rent
expense.
|
|
In
connection with the Asset Purchase Agreement (Note 11), XTL
Biopharmaceuticals Ltd. has assumed the commitment to the Valley
Cottage
lease.
|
(Continued)
F-66
VIVOQUEST,
INC.
(A
DEVELOPMENT STAGE ENTERPRISE)
NOTES
TO
FINANCIAL STATEMENTS
(INFORMATION
WITH RESPECT TO THE SIX MONTH PERIOD
ENDED
JUNE 30, 2004 AND THE PERIOD SUBSEQUENT TO
DECEMBER
31, 2004 IS UNAUDITED)
| 8. |
Commitments
and Contingencies (Continued):
|
| (b) |
Convertible
Notes
|
|
During
2001 and 2002, the Company obtained additional financing through
the
issuance of short term convertible term notes (the “Bridge Notes”)
totaling approximately $10.4 million, which accrue interest at
a rate of
6% per year. Principal plus accrued interest on the Bridge Notes,
as
amended in November 2002 (the “November Amendment”), were due on December
31, 2003. The Bridge Notes, as amended, are convertible into the
Company’s
Preferred Stock as follows: (i) if the Company consummated a convertible
preferred stock financing with one or more investors, that is approved
by
certain of the holders of the Bridge Notes, on or before December
31, 2003
(the “Qualifying Financing”), then, simultaneously with the closing of
such Qualifying Financing, the outstanding principal and accrued
interest
on the Bridge Notes would be converted into shares of the new series
of
convertible preferred stock of the Company which is authorized
by the
Company in connection with the Qualifying Financing at a price
per share
equal to that paid by investors in the Qualifying Financing; or
(ii) if a
Qualifying Financing is not obtained by such date, the Bridge Notes
and
accrued interest would be converted into shares of the Company’s B
preferred at $2.625 per share. Although the November Amendment
extended
the due date of the Bridge Notes to December 31, 2003, all other
rights
and privileges of the holders of the Bridge Notes remained unchanged.
The
extension of the due date of the Bridge Notes specified in the
November
Amendment resulted in a substantial change in the Bridge Notes
in
accordance with EITF 96-19, “Debtor’s Accounting for a Modification or
Exchange of Debt Instruments.” Accordingly, the Company recognized a loss
on extinguishment of debt in the amount of $350,450, which represented
the
difference between the fair value and carrying amount of the Bridge
Notes
at November 19, 2002, the date of the November Amendment. A total
of
approximately $4.9 million of the Bridge Notes were sold to five
related
parties. During March 2003, following a Qualifying Financing, all
Bridge
Notes were converted to shares of Series C Preferred Stock (see
Note
6).
|
(Continued)
F-67
VIVOQUEST,
INC.
(A
DEVELOPMENT STAGE ENTERPRISE)
NOTES
FOR
FINANCIAL STATEMENTS
(INFORMATION
WITH RESPECT TO THE SIX MONTH PERIOD
ENDED
JUNE 30, 2004 AND THE PERIOD SUBSEQUENT TO
DECEMBER
31, 2004 IS UNAUDITED)
| 8. |
Commitments
and Contingencies (Continued):
|
| (b) |
Convertible
Notes (Continued)
|
|
In
connection with the sale of the Bridge Notes, the Bridge Note holders
received fully exercisable warrants (“Bridge Warrants”) to purchase shares
of the Company’s preferred stock sold in the next round of financing at
the price paid by investors in that round of financing or to purchase
shares of B Preferred at $2.625 per share as defined. A total of
659,421
Bridge Warrants were issued in 2001. As the result of the issuance
of
Series C Preferred Stock, as discussed in Note 7, the terms of
the 2001
Bridge Warrants were fixed, so that the 2001 Bridge Warrants holders
would
be able to purchase 3,243,517 shares of Series C Preferred Stock
at a
price of $0.53368 per share. An additional 605,714 Bridge Warrants
were
issued in 2002. Bridge Warrants expire after 10 years. According
to the
November Amendment, if the Company received at least $3.5 million
from
certain defined investors (the “Investors”) in debt or equity financing on
or before December 31, 2002, the Bridge Warrants issued in 2002
would
terminate and not be exercisable. The Company raised $4.1 million
from the
Investors as of December 31, 2002 and thus all 2002 Bridge Warrants
expired on that date. The aggregate fair value of the Bridge Warrants
issued in 2001 and 2002 on the dates of issue was $1,177,366 and
$475,987,
respectively, which was equal to the discount on the respective
Bridge
Notes. Such discount was amortized on a straight-line basis, which
approximates the interest method, over the original term of the
Bridge
Notes.
|
| (c) |
Collaboration
Agreements
|
|
In
order to further its research and development efforts, the Company
has
entered into several consulting and collaboration agreements with
individuals, research institutes and
universities.
|
| (i) |
Scientific
Advisors
|
The
Company has assembled a number of scientists (the “Scientists”) from leading
universities in the United States and Hong Kong, some of whom serve on the
Company’s Scientific Advisory Board. The Scientists provide advice to the
Company regarding relevant science, research strategy, evaluation of potential
lead candidates and intellectual property.
(Continued)
F-68
VIVOQUEST,
INC.
(A
DEVELOPMENT STAGE ENTERPRISE)
NOTES
TO
FINANCIAL STATEMENTS
(INFORMATION
WITH RESPECT TO THE SIX MONTH PERIOD
ENDED
JUNE 30, 2004 AND THE PERIOD SUBSEQUENT TO
DECEMBER
31, 2004 IS UNAUDITED)
| 8. |
Commitments
and Contingencies (Continued):
|
|
(i)
|
Scientific
Advisors (Continued)
|
|
During
2000, 2001, and 2002, the Company entered into consulting agreements
(the
“Scientists Agreements”) with each of the Scientists, which provide for
monetary compensation and the sale to each Scientist of shares
of the
Company’s Common Stock at $0.025 and $0.13125 per share which was the fair
value of the Company’s Common Stock on the date of sale in 2001 and 2002,
respectively. During 2004 and 2003, the Company entered into consulting
agreements which provided for monetary
compensation.
|
|
The
Company has recognized expenses with regard to the Scientists Agreements
totaling approximately $165,000, $114,000 and $208,000 for the
six months
ended June 30, 2005 and 2004 and the year ended December 31, 2004 and
$1,192,000 for the cumulative period from September 29, 1998 (inception)
to June 30, 2005. In addition, as discussed in Note 5, the Company
has
notes receivable of $66,500, $66,500 and $53,375 at December 31,
2003,
2002 and 2001, respectively, from the sale of Common Stock to the
Scientists. The Scientists Agreements expire after one year and
may be
extended upon mutual agreement of the Company and Scientists. Either
party
may terminate the Scientists Agreements upon thirty days written
notice.
As of December 31, 2004, all of the Scientists Agreements have been
verbally extended.
|
| (ii) |
Hong
Kong University of Science and
Technology
|
|
Between
1999 and 2001, the Company and the Biotechnology Research Institute
(“BRI”) of the Hong Kong University of Science and Technology (“HKUST”)
entered into several collaboration
and license agreements,
whereby BRI would provide laboratory facilities and know-how to
enhance
the Company’s research efforts. During the years ended December 31, 1999,
2000 and 2001, the Company made payments to BRI under these agreements.
Total payments recognized by the Company during 2001 and 2002 were
approximately $38,000 and $84,000, respectively. During the year
ended
December 31, 2003, the parties decided to terminate all agreements
and at
December 31, 2003, there were no remaining obligations on the part
of
either party under these
agreements.
|
(Continued)
F-69
VIVOQUEST,
INC.
(A
DEVELOPMENT STAGE ENTERPRISE)
NOTES
TO
FINANCIAL STATEMENTS
(INFORMATION
WITH RESPECT TO THE SIX MONTH PERIOD
ENDED
JUNE 30, 2004 AND THE PERIOD SUBSEQUENT TO
DECEMBER
31, 2004 IS UNAUDITED)
| 8. |
Commitments
and Contingencies (Continued):
|
| (ii) |
Hong
Kong University of Science and Technology
(Continued)
|
|
In
June 2004, the Company and the Biotechnology Research Institute
(“BRI”) of
the Hong Kong University of Science and Technology (“HKUST”) entered into
a new collaboration agreements called “Screen Library” program. The
program will be carried out within 9 months from the effective
date June
2004 and can be extended for additional 6 months. Under the agreement,
the
Company agrees to pay HK$ 200,000 to BRI for conducting the screening
activity. As of December 31, 2004, no payment has been made to
BRI and the
Company has not recognized any expenses relating to this
agreement.
|
| (iii) |
Aaron
Diamond AIDS Research
Center
|
|
In
February 2001, the Company entered into a research agreement with
the
Aaron Diamond AIDS Research Center (“Aaron Diamond”) to undertake a
collaborative research program, under which Aaron Diamond will
develop
assays for screening of mutually agreed upon natural and other
product
extracts, chemical compounds and libraries, provided by the Company,
for
human immunodeficiency virus (HIV) activity. The Company will retain
all
rights to any inventions or products arising from the research
program and
will have the right to obtain patents thereon. The term of the
Aaron
Diamond agreement is for a period of five years from the date of
execution, unless extended by written agreement between the parties,
except that either party may terminate the Aaron Diamond agreement
on
thirty days prior written notice. During the term of the Aaron
Diamond
agreement, the research program will be reviewed by the Company
on an
annual basis and the research continued subject to the approval
of the
Company. During the years ended December 31, 2001 and 2002, the
Company
approved budgets for the research program for one-year periods
ending
February 2002 and February 2003, respectively. For the years ended
December 31, 2003, 2002 and 2001, the Company recognized $161,000,
$499,000 and $410,000, respectively, as research and development
expenses
in connection with the Aaron Diamond agreement. The Aaron Diamond
agreement has not been extended beyond February
2003.
|
(Continued)
F-70
VIVOQUEST,
INC.
(A
DEVELOPMENT STAGE ENTERPRISE)
NOTES
TO
FINANCIAL STATEMENTS
(INFORMATION
WITH RESPECT TO THE SIX MONTH PERIOD
ENDED
JUNE 30, 2004 AND THE PERIOD SUBSEQUENT TO
DECEMBER
31, 2004 IS UNAUDITED)
| 8. |
Commitments
and Contingencies (Continued):
|
| (iv) |
Peking
University
|
In
February 2001, the Company entered into a research agreement (the “Peking
Agreement”) with Peking University in China to undertake a collaborative
research program, under which Peking University will develop the methodologies
to synthesize natural product-like molecules for viral and other therapeutic
targets. Such molecules will be screened by the Company for activity against
those targets. The Company will retain all rights to any inventions or products
arising from the research program and will have the right to obtain patents
thereon. The Company will provide to Peking University, an amount not to
exceed
$100,000 per year, payable quarterly, in support of defined, direct and indirect
costs of the research program. The term of the agreement is for a period
of
three years from the date of execution, unless extended by written agreement
between the parties, except that either party may terminate this agreement
on
thirty days prior written notice. The research program will be reviewed by
the
Company on an annual basis and the research continued subject to the approval
of
the Company. For the years ended December 31, 2004 and for the six months
ended
June 30, 2004 and 2005, the Company recognized $25,000, $25,000 and
$20,000, respectively, as research and development expenses in connection
with
the Peking Agreement.
| (v) |
Inpharmatica
Ltd.
|
|
In
June 2004, the Company and Inphamatica Ltd. entered into a “service
agreement” whereby Inphamatica will undertaken certain services such as
screening services, profiling services, consultancy services, modelling
services and other. The service will be carried out over a fixed
period of
24 months commencing from June 1, 2004. The service fees shall
be paid in
accordance with payment schedule specified in the agreement. For
the years
ended December 31, 2004 and for the six months ended June 30, 2004
and
2005, the Company has recognized expenses with regard to the “service
agreement” totalling approximately $115,000, $nil, and $58,000,
respectively.
|
(Continued)
F-71
VIVOQUEST,
INC.
(A
DEVELOPMENT STAGE ENTERPRISE)
NOTES
TO
FINANCIAL STATEMENTS
(INFORMATION
WITH RESPECT TO THE SIX MONTH PERIOD
ENDED
JUNE 30, 2004 AND THE PERIOD SUBSEQUENT TO
DECEMBER
31, 2004 IS UNAUDITED)
| 8. |
Commitments
and Contingencies (Continued):
|
|
(vi)
|
Beijing
Kaizheng Biotech Developing
Ltd.
|
|
In
March 2004, the Company and Beijing Kaizheng
Biotech
Developing Ltd. entered into a “Contract Screening Agreement”. The
screening program consists of individual projects whereby Kaizheng
will
provide research equipment, reagents and personnel to conduct its
screening program at its Beijing facility. The service will be
carried out
over a fixed period of 24 months commencing from June 1, 2004.
The Company
agrees to pay Kaizheng Project fees specified in applicable project
description. During 2004, the Company has not recognized any expenses
with
regard to this agreement.
|
| (vii) |
Replizyme
Ltd.
|
|
In
February 2004, the Company and Replizyme Ltd. entered into a “Service
Agreement”. Replizyme will screen compounds from Vivoquest for activity
against Hepatitis C Polymerase. The maximum cost for these tests
is
approximately $6,000. During 2004, the Company has not recognized
any
expenses with regard to this
agreement.
|
| (viii) |
New
York Medical College and David Frick,
PHD.
|
|
In
April 2004, the Company and New York Medical College entered into
a
“Material Transfer Agreement” whereby NYMC will perform material testings
for the Company. The Company agrees to pay NYMC $6,200 payable
in three
instalments as specified in the agreement. Payments for the years
ended
December 31, 2004 and for the six months ended June 30, 2004 and
2005,
which have been paid and recognized by the Company are $6,200,
$2,000 and
$nil, respectively.
|
(Continued)
F-72
VIVOQUEST,
INC.
(A
DEVELOPMENT STAGE ENTERPRISE)
NOTES
TO
FINANCIAL STATEMENTS
(INFORMATION
WITH RESPECT TO THE SIX MONTH PERIOD
ENDED
JUNE 30, 2004 AND THE PERIOD SUBSEQUENT TO
DECEMBER
31, 2004 IS UNAUDITED)
| 8. |
Commitments
and Contingencies (Continued):
|
|
(ix)
|
University
of Colorado
|
|
In
April 2004, the Company and University of Colorado entered into
a
“Material Transfer Agreement” whereby The University of Colorado will
perform material testing’s for the Company. The Company agrees to pay
$5,000 payable in three instalments as specified in the agreement,
which
have been paid and recognized by the Company during
2004.
|
| 9. |
Stock
Plan:
|
|
On
September 23, 1999, the Company adopted the 1999 Stock Plan (the
“Plan’)
whereby the Board of Directors of the Company (the “Board”) may grant (i)
options to purchase shares of Common Stock (“Options”) or (ii) Common
Stock (“Grant Stock”) to employees, officers, and directors of and
consultants and advisors to the Company. The Plan provides for
the
issuance of up to 6,869,047
shares
of Common Stock. Such amount is subject to adjustment for stock
splits,
stock dividends and other capital adjustments, as defined. All
Options
granted under the Plan are intended to be non-qualified unless
specified
by the Board to be incentive stock options (“ISO”), as defined by the
Internal Revenue Code. ISO’s may only be granted to employees of the
Company and may not be granted at exercise prices below fair value
of the
Common Stock on the date of grant (110% of fair value for employees
who
own 10% or more of the Company). Nonqualified Options may be granted
to
participants at less than the fair value of the Common Stock on
the date
of grant. The Board determines the terms upon which the Options
vest as
well as the exercise price of each Option grant. Options usually
vest over
4 years. The Board determines whether shares of Grant Stock are
subject to
restrictions and the terms by which such restrictions vest. Unvested
shares of Grant Stock may be subject to forfeiture upon termination
of
employment or occurrence of other events. The period during which
an
Option may be exercised may not exceed ten years from the date
of grant
(five years for grants of ISO’s to employees who own 10% or more of the
Company) and under certain situations, the Option’s expiration date may be
accelerated. The Plan terminates on September 23,
2009.
|
(Continued)
F-73
VIVOQUEST,
INC.
(A
DEVELOPMENT STAGE ENTERPRISE)
NOTES
TO
FINANCIAL STATEMENTS
(INFORMATION
WITH RESPECT TO THE SIX MONTH PERIOD
ENDED
JUNE 30, 2004 AND THE PERIOD SUBSEQUENT TO
DECEMBER
31, 2004 IS UNAUDITED)
| 9. |
Stock
Plan (Continued):
|
|
The
following table summarizes stock option activity from the inception
of the
plan through June 30, 2005:
|
|
Number
of
|
Average
|
Number
of
|
Average
|
||||||||||
|
Options
|
Exercise
|
Options
|
Exercise
|
||||||||||
|
Outstanding
|
Price
|
Exercisable
|
Price
|
||||||||||
|
Balance
outstanding at January 1, 2004
|
2,427,500
|
$
|
0.09
|
737,363
|
$
|
0.12
|
|||||||
|
2004:
Granted
|
390,000
|
0.13
|
|||||||||||
|
2004:
Forfeited
|
(105,000
|
)
|
(0.10
|
)
|
|||||||||
|
Balance
outstanding at June 30, 2004
|
2,712,500
|
0.10
|
632,363
|
0.12
|
|||||||||
|
2004:
Granted
|
620,000
|
0.13
|
|||||||||||
|
2004:
Forfeited
|
(87,000
|
)
|
(0.06
|
)
|
|||||||||
|
Balance
outstanding at December 31, 2004
|
3,245,500
|
0.11
|
933,019
|
0.08
|
|||||||||
|
Stock
options forfeited
|
(251,250
|
)
|
(0.09
|
)
|
|||||||||
|
Stock
options exercised
|
(13,750
|
)
|
(0.13
|
)
|
|||||||||
|
Balance
outstanding at June 30, 2005
|
$
|
2,980,500
|
$
|
0.13
|
768,019
|
0.11
|
|||||||
(Continued)
F-74
VIVOQUEST,
INC.
(A
DEVELOPMENT STAGE ENTERPRISE)
NOTES
TO
FINANCIAL STATEMENTS
(INFORMATION
WITH RESPECT TO THE SIX MONTH PERIOD
ENDED
JUNE 30, 2004 AND THE PERIOD SUBSEQUENT TO
DECEMBER
31, 2004 IS UNAUDITED)
| 9. |
Stock
Plan (Continued):
|
|
For
all periods presented, the exercise price of options granted to
employees
was equal to the fair value of the Company’s common stock on the date of
grant. At December 31, 2004, and June 30, 2005 3,623,547 and 3,888,547,
respectively, shares of Common Stock were available for future
grant under
the Plan.
|
|
The
following table summarizes stock option information as of June
30,
2005:
|
|
Options
Outstanding
|
Options
Exercisable
|
|||||||||||||||
|
Weighted
|
Weighted
|
Weighted
|
||||||||||||||
|
Range
of
|
Average
|
Average
|
Average
|
|||||||||||||
|
Exercise
|
Number
|
Remaining
|
Exercise
|
Number
|
Exercise
|
|||||||||||
|
Prices
|
Outstanding
|
Contractual
Life
|
Price
|
Exercisable
|
Price
|
|||||||||||
|
$
0.06
|
1,122,500
|
6.8
|
$
|
0.06
|
42,750
|
$
|
0.06
|
|||||||||
|
0.13
-0.13125
|
1,858,000
|
8.2
|
0.13
|
725,269
|
0.13
|
|||||||||||
|
$0.06-$0.13125
|
2,980,500
|
7.7
|
$
|
0.10
|
768,019
|
$
|
0.11
|
|||||||||
| 10. |
Income
Taxes:
|
|
Since
inception there had been no provision (benefit) for federal or
state
income taxes because the Company has incurred operating losses
and has
established valuation allowances equal to the total deferred tax
asset.
|
(Continued)
F-75
VIVOQUEST,
INC.
(A
DEVELOPMENT STAGE ENTERPRISE)
NOTES
TO
FINANCIAL STATEMENTS
(INFORMATION
WITH RESPECT TO THE SIX MONTH PERIOD
ENDED
JUNE 30, 2004 AND THE PERIOD SUBSEQUENT TO
DECEMBER
31, 2004 IS UNAUDITED)
| 10. |
Income
Taxes (Continued):
|
|
The
tax effect of temporary differences and net operating losses as
of June
30, 2005 and December 31, 2004 are as
follows:
|
|
June
30,
|
December
31,
|
||||||
|
2005
|
2004
|
||||||
|
Deferred
tax assets and valuation allowance:
|
|||||||
|
Net
operating loss carryforwards
|
$
|
6,883,686
|
$
|
5,905,286
|
|||
|
Capitalized
costs
|
2,474,920
|
2,227,775
|
|||||
|
Depreciation
and amortization
|
313,836
|
304,138
|
|||||
|
Research
and experimentation tax credit carry forward
|
168,336
|
168,336
|
|||||
|
Valuation
allowance
|
(9,840,778
|
)
|
(8,605,535
|
)
|
|||
|
|
$ |
—
|
$
|
—
|
|||
|
As
of December 31, 2004, the Company has available, for tax purposes,
unused
net operating loss carryforwards of approximately $14.8 million,
which
will expire between 2019 and 2022. Future ownership changes may
limit the
future utilization of these net operating loss carryforwards as
defined by
the federal and state tax codes.
|
|
11.
|
Subsequent
Events:
|
|
In
August 2005, the Company entered into an asset purchase agreement
(“Asset
Purchase Agreement”) to sell substantially all of its tangible operating
assets to XTL Biopharmaceuticals Inc. (“XTL Inc.”), a Delaware
corporation, in consideration for approximately $450,000 in ordinary
shares, of XTL Biopharmaceuticals Ltd., an Israeli corporation
(“XTL”),
and the parent of XTL Inc. In addition, pursuant to an interim
funding
letter, XTL Inc. provided $400,000 to the Company to cover operating
expenses prior to the closing of the transaction. The book gain
on sale of
the assets related to this transaction was approximately $434,000.
The
Company’s shares of common and preferred stock and convertible secured
promissory notes payable (see Note 5) were not part of this
transaction.
|
(Continued)
F-76
VIVOQUEST,
INC.
(A
DEVELOPMENT STAGE ENTERPRISE)
NOTES
TO
FINANCIAL STATEMENTS
(INFORMATION
WITH RESPECT TO THE SIX MONTH PERIOD
ENDED
JUNE 30, 2004 AND THE PERIOD SUBSEQUENT TO
DECEMBER
31, 2004 IS UNAUDITED)
|
11.
|
Subsequent
Events (Continued):
|
|
In
August 2005, the Company also entered into a Licensing Agreement
(“License
Agreement”) with XTL, pursuant to which the Company granted to XTL
exclusive worldwide rights to the Company’s intellectual property and
technology. The terms of the License Agreement included an initial
upfront
license fee of approximately $941,000 which was paid in ordinary
shares of
XTL stock. The License Agreement also provides for additional milestone
payments triggered by certain regulatory and sales targets. These
milestone payments could total $34.6 million, $25.0 million of
which would
be due upon or following regulatory approval or actual products
sales, and
are payable in cash or ordinary shares of XTL at its election.
In
addition, the License Agreement requires that XTL make royalty
payments on
products sales.
|
|
The
Asset Purchase Agreement and the License Agreement with VivoQuest
was
completed in September 2005. None of these milestones have
been reached as of June 30,
2005.
|
|
All
shares of stock of XTL received in the Asset Purchase Agreement
and
License Agreement were subsequently sold for a net loss of approximately
$160,000, which loss has not been recorded in the attached financial
statements.
|
|
An
agreement regarding distribution of proceeds has been entered into
by the
Company whereas any proceeds from the asset sale, net of liabilities
and
costs of the Company shall be distributed in the ratio of 91.3%
to the
holders of the Convertible Secured Promissory Notes Payable (see
Note 5)
and 8.7% to the remaining incentive pool (employees of the Company
at the
time of the closing of the asset sale) pro rata in proportion to
their
option shares at the time of the closing. As of January 2006,
approximately $900,000 has been distributed in
total.
|
|
In
September 2005, the Company approved a plan to dissolve and liquidate
on
or before September 2006.
|
F-77
PROSPECTUS
April
20, 2006
XTL
Biopharmaceuticals Ltd.
7,000,000.5
American Depositary Shares
Representing
Ten Ordinary Shares
PART
II — INFORMATION NOT REQUIRED IN PROSPECTUS
ITEM
6. INDEMNIFICATION
OF DIRECTORS AND OFFICERS.
Israeli
law permits a company to insure an office holder in respect of liabilities
incurred by him or her as a result of an act or omission in the capacity of
an
office holder for:
|
·
|
a
breach of the office holder’s duty of care to the company or to another
person;
|
|
·
|
a
breach of the office holder’s fiduciary duty to the company, provided that
he or she acted in good faith and had reasonable cause to believe
that the
act would not prejudice the company; and
|
|
·
|
a
financial liability imposed upon the office holder in favor of another
person.
|
Moreover,
a company can indemnify an office holder for any of the following obligations
or
expenses incurred in connection with the acts or omissions of such person in
his
or her capacity as an office holder:
|
·
|
monetary
liability imposed upon him or her in favor of a third party by a
judgment,
including a settlement or an arbitral award confirmed by the court;
and
|
|
·
|
reasonable
litigation expenses, including attorneys’ fees, actually incurred by the
office holder or imposed upon him or her by a court, in a proceeding
brought against him or her by or on behalf of the company or by a
third
party, or in a criminal action in which he or she was acquitted,
or in a
criminal action which does not require criminal intent in which he
or she
was convicted; furthermore, a company can, with a limited exception,
exculpate an office holder in advance, in whole or in part, from
liability
for damages sustained by a breach of duty of care to the
company.
|
The
Registrant’s Articles of Association allow for insurance, exculpation and
indemnification of office holders to the fullest extent permitted by law. The
Registrant has entered into indemnification, insurance and exculpation
agreements with its directors and executive officers, following shareholder
approval of these agreements. The Registrant has directors’ and officers’
liability insurance covering its officers and directors for a claim imposed
upon
them
as a result of an action carried out while serving as an officer or director,
for (a) the breach of duty of care towards the Registrant or towards another
person, (b) the breach of fiduciary duty towards the Registrant, provided that
the officer or director acted in good faith and had reasonable grounds to assume
that the action would not harm the Registrant’s interests, and (c) a monetary
liability imposed upon him in favor of a third party.
ITEM
7. RECENT
SALES OF UNREGISTERED SECURITIES.
The
following is a summary transactions by the Registrant in the last three years
involving sales of the Registrant’s securities that were not registered under
the Securities Act of 1933.
VivoQuest
Transaction
In
September 2005, the Registrant licensed from VivoQuest, Inc., a US
privately-held company which is a development stage enterprise, exclusive
worldwide rights to VivoQuest’s intellectual property and technology, covering a
proprietary compound library, including VivoQuest’s lead hepatitis C compounds.
In addition, the Registrant acquired from VivoQuest certain assets, including
VivoQuest’s laboratory equipment, assumed VivoQuest’s lease of its laboratory
space and certain research and development employees. In connection with the
VivoQuest transaction, the Registrant: (1) issued 1,314,420 of its ordinary
shares with an aggregate value of $1,391,000 (calculated based upon the average
of the closing prices per share for the period commencing two days before,
and
ending two days after, the closing of the transaction); (2) paid approximately
$400,000 to VivoQuest to fund certain of their operating expenses prior to
the
closing of the transaction, and incurred $148,000 in direct expenses associated
with the transaction; (3) agreed to make additional contingent milestone
payments triggered by certain regulatory and sales targets, totaling up to
$34.6
million, $25.0 million of which will be due upon or following regulatory
approval or actual product sales, which are payable in cash or ordinary shares
at the Registrant’s election; and (4) agreed to make royalty payments on future
product sales. The ordinary shares issued in connection with the VivoQuest
transaction were issued in reliance on the exemption from registration afforded
by the provisions of Section 4(2) under the Securities Act.
Option
Grants
In
2003,
in return for services provided to the Registrant, the Registrant granted to
an
employee options to purchase a total of 125,000 ordinary shares at an exercise
price of $0.250 per option. These options were granted under the same terms
and
conditions as the Registrant’s plan or non-plan grants. The options were granted
to the employee in reliance on the exemption from registration afforded by
the
provisions of Section 4(2) under the Securities Act.
In
2004,
in return for services provided to the Registrant, the Registrant granted to
a
director, certain employees, and consultants, options to purchase a total of
560,000 ordinary shares at an exercise price between $0.20 and $0.486 per
option. These options were granted under the same terms and conditions as the
Registrant’s plan or non-plan grants. The options were granted to the director,
employees and consultants in reliance on the exemption from registration
afforded by the provisions of Section 4(2) under the Securities
Act.
In
August
2005, in return for service as the Chairman of the Board, the Registrant’s
shareholders granted Michael S. Weiss options to purchase a total of 9,250,000
ordinary shares at an exercise price equal to $0.354 per share. These options
are exercisable for a period of five years from the date of issuance, and were
granted under the same terms and conditions as the Registrant’s Share Option
Plan 2001. The options shall vest upon achievement of certain market
capitalization based milestones recommended by the Audit Committee and set
by
the Registrant’s Board of Directors and approved by the shareholders at the
Registrant’s annual shareholders’ meeting in August 2005. The options were
granted to the Chairman in reliance on the exemption from registration afforded
by the provisions of Section 4(2) under the Securities Act.
In
August
2005, in return for service as non-executive directors, the Registrant’s
shareholders approved grants to William Kennedy and Jonathan Spicehandler of
60,000 options each, having an exercise price equal to $0.853 per share, vesting
over the three years from the date of grant, and furthermore approved three
annual grants of 20,000 options each, at an exercise price equivalent to the
then current closing price of the Registrant’s ADRs on the Nasdaq Stock Market
(subject to the ordinary share-ADR ratio). The options were granted to the
non-executive directors in reliance on the exemption from registration afforded
by the provisions of Section 4(2) under the Securities Act.
In
March
2006, the Registrant’s board of directors granted Ron Bentsur, Chief Executive
Officer, options to purchase a total of 7,000,000 ordinary shares at an exercise
price equal to $0.774 per share (closing price of the last trading day prior
to
official appointment). These options are exercisable for a period of ten years
from the date of issuance, and granted under the same terms and conditions
as
the Share Option Plan 2001 and any option agreement entered into with Mr.
Bentsur. Of these, 2,333,334 options shall vest as follows: 777,782 options
on
the one-year anniversary of the issuance of the options and 194,444 options
at
the end of each quarter thereafter for the following two years. The balance
of
options shall vest upon achievement of certain milestones (2,333,333 upon the
achievement of $350 million market capitalization or $75 million in working
capital, as set out in the agreement and 2,333,333 upon the achievement of
$550
million market capitalization or $125 million in working capital, as set out
in
the agreement). The options were granted to the Registrant’s Chief Executive
Officer in reliance on the exemption from registration afforded by the
provisions of Section 4(2) under the Securities Act.
In
March
2006, the Registrant’s board of directors also approved grants of a total of
9,898,719 options to Michael S. Weiss, the Chairman of the Board of Directors.
These options are exercisable at an exercise price which is the volume weighted
average price per share of the ADRs on Nasdaq during the thirty trading days
prior to the board of directors’ approval divided by ten, or $0.713. The options
shall vest as follows: (i) 1/3 of such options shall vest over three years,
of
which amounts, 1/3 shall vest and be exercisable upon the first anniversary
of
the issuance of the options and the remainder shall vest and be exercisable
on a
quarterly basis; (ii) 1/3 of such options shall vest and be exercisable upon
the
Registrant achieving a total market capitalization on a fully diluted basis
of
more than US $350 million; and (iii) 1/3 of such options shall vest upon the
Registrant achieving a total market capitalization on a fully diluted basis
of
more than US $550 million. The options can be exercised for a period of ten
years. The grant of such options is conditional upon approval of the
shareholders at a duly convened shareholder meeting expected to take place
later
this year. The options were granted to the Chairman in reliance on the exemption
from registration afforded by the provisions of Section 4(2) under the
Securities Act.
ITEM
8. EXHIBITS
AND FINANCIAL STATEMENT SCHEDULES.
The
following exhibits are filed as part of this Registration Statement:
|
Exhibit
Number
|
Description
|
|
|
1.1
|
Form
of Securities Purchase Agreement, dated March 17, 2006, by and among
XTL
Biopharmaceuticals Ltd., and the purchasers named
therein.
|
|
|
1.2
|
Form
of Registration Rights Agreement, dated March 22, 2006, by and among
XTL
Biopharmaceuticals Ltd. and the purchasers named
therein.
|
|
|
1.3
|
Form
of Ordinary Share Purchase Warrants, dated March 22, 2006, issued
to the
purchasers under the Securities Purchase Agreement.
|
|
|
1.4
|
Escrow
Agreement, dated March 22, 2006, by and among XTL Biopharmaceuticals
Ltd.,
the Placement Agents named therein, and JPMorgan Chase Bank, N.A., as
escrow agent.
|
|
|
3.1
|
Articles
of Association†
|
|
|
4.1
|
Form
of Share Certificate†
|
|
|
4.2
|
Form
of American Depositary Receipt (included in Exhibit 4.3)
†
|
|
|
4.3
|
Deposit
Agreement, dated as of August 31, 2005, by and between XTL
Biopharmaceuticals Ltd., The Bank of New York, as Depositary, and
each
holder and beneficial owner of American Depositary Receipts issued
thereunder†
|
|
|
4.5
|
Form
of Director and Senior Management Lock−up Letter
|
|
|
5.1
|
Opinion
of Kantor & Co. regarding legality of the ADRs
|
|
|
10.1
|
Research
and License Agreement Between Yeda Research and Development Company
Ltd.
and Xenograft Technologies Ltd. dated April 7, 1993†
|
|
|
10.2
|
Amendment
of Research and License Agreement Between Yeda Research and Development
Company Ltd. and XTL Biopharmaceuticals Ltd. dated August 31,
1995†
|
|
|
10.3
|
Second
Extension Agreement Between Yeda Research and Development Company
Ltd. and
XTL Biopharmaceuticals Ltd. dated August 14, 1996†
|
|
|
10.4
|
Third
Extension Agreement Between Yeda Research and Development Company
Ltd. and
XTL Biopharmaceuticals Ltd. dated November 25, 1997†
|
|
|
10.5
|
Amendment
No. 2 to Research and License Agreement dated April 7, 1993, as amended
on
August 31, 1995, between Yeda Research and Development Company Ltd.
and
XTL Biopharmaceuticals Ltd. dated January 25, 1998†
|
|
|
10.6
|
Amendment
No. 3 to Research and License Agreement dated April 7, 1993 between
Yeda
Research and Development Company Ltd. and XTL Biopharmaceuticals
Ltd.
dated January 26, 2003†
|
|
|
10.7
|
Amendment
No. 4 to Research and License Agreement dated April 7, 1993 between
Yeda
Research and Development Company Ltd. and XTL Biopharmaceuticals
Ltd.
dated June 2, 2004†
|
|
|
10.8
|
License
Agreement Between XTL Biopharmaceuticals Ltd. and Cubist
Biopharmaceuticals, Inc., dated June 2, 2004†
|
|
|
10.9
|
License
Agreement Between XTL Biopharmaceuticals Ltd. and DRK-Blutspendedienst
Baden-Wurttemberg (Ulm University, Germany) dated April 18,
2000†
|
|
|
10.10
|
License
Agreement Between XTL Biopharmaceuticals Ltd. and Stanford University,
dated September 12, 2003†
|
|
|
10.11
|
License
Agreement Between XTL Biopharmaceuticals Ltd. and Applied Immunogenetics
LLC, dated September 12, 2003†
|
|
|
10.12
|
1998
Share Option Plan dated October 19, 1998†
|
|
|
10.13
|
1999
Share Option Plan dated June 1, 1999†
|
|
|
10.14
|
1999
International Share Option Plan Dated June 1, 1999†
|
|
|
10.15
|
2000
Share Option Plan dated April 12, 2000†
|
|
|
10.16
|
2001
Share Option Plan dated February 28, 2001†
|
|
|
10.17
|
Letter
of Understanding, dated August 5, 2005, relating to the License Agreement
dated June 2, 2004 between Cubist Pharmaceuticals, Inc. and XTL
Biopharmaceuticals Ltd.†
|
|
10.18
|
License
Agreement, dated February 26, 2003, between XTL Biopharmaceuticals
Ltd.
and B&C Biopharm Co., Ltd. †
|
|
|
10.19
|
Employment
Agreement, dated August 1, 1999, between XTL Biopharmaceuticals Ltd.
and
Jonathan Burgin†
|
|
|
10.20
|
Employment
Agreement, dated as of January 3, 2006, between XTL Biopharmaceuticals
Ltd. and Ron Bentsur
|
|
|
10.21
|
Agreement,
dated August 1, 2005, between XTL Biopharmaceuticals Ltd. and Michael
S.
Weiss†
|
|
|
10.22
|
Form
No. 1 of Director Service Agreement†
|
|
|
10.23
|
Form
No. 2 of Director Service Agreement†
|
|
|
10.24
|
Form
No. 3 of Director Service Agreement†
|
|
|
10.25
|
Form
No. 4 of Director Indemnification Agreement†
|
|
|
10.26
|
License
Agreement Between XTL Biopharmaceuticals Ltd. and VivoQuest, Inc.,
dated
August 17, 2005†
|
|
|
10.27
|
Asset
Purchase Agreement Between XTL Biopharmaceuticals Ltd. and VivoQuest,
Inc., dated August 17, 2005†
|
|
|
21.1
|
List
of Subsidiaries†
|
|
|
23.1
|
Consent
of Kantor & Co. (included in Exhibit 5.1)
|
|
|
23.2
|
Consent
of Kesselman & Kesselman, a member of PricewaterhouseCoopers
International Ltd, dated April 20, 2006.
|
|
|
23.3
|
Consent
of PricewaterhouseCoopers LLP, dated April 20, 2006.
|
|
|
23.4
|
Consent
of Cornick, Garber & Sandler, LLP, dated April 20,
2006.
|
|
|
23.5
|
Consent
of Somekh Chaikin, a member firm of KPMG International, dated April
20,
2006
|
|
|
24.1
|
Power
of Attorney (included in the signature page
hereto)
|
†
Incorporated by reference from the registration statement on Form 20-F filed
by
XTL Biopharmaceuticals Ltd. with the Securities and Exchange Commission on
July
14, 2005, as it may be amended or restated.
ITEM
9. UNDERTAKINGS.
The
undersigned Registrant hereby undertakes that, for purposes of determining
any
liability under the Securities Act of 1933, each filing of the Registrant's
annual report pursuant to section 13(a) or section 15(d) of the Securities
Exchange Act of 1934 (and, where applicable, each filing of an employee benefit
plan's annual report pursuant to section 15(d) of the Securities Exchange Act
of
1934) that is incorporated by reference in the registration statement shall
be
deemed to be a new registration statement relating to the securities offered
therein, and the offering of such securities at that time shall be deemed to
be
the initial bona fide offering thereof.
Insofar
as indemnification for liabilities arising under the Securities Act may be
permitted to directors, officers and controlling persons of the Registrant
pursuant to the foregoing provisions, or otherwise, the Registrant has been
advised that in the opinion of the Securities and Exchange Commission such
indemnification is against public policy as expressed in the Securities Act
and
is, therefore unenforceable. In the event that a claim for indemnification
against such liabilities (other than the payment by the Registrant of expenses
incurred or paid by a director, officer or controlling person of the Registrant
in the successful defense of any action, suit or proceeding) is asserted by
such
director, officer or controlling person in connection with the securities being
registered, the Registrant will, unless in the opinion of its counsel the matter
has been settled by controlling precedent, submit to a court of appropriate
jurisdiction the question of whether such indemnification by it is against
public policy as expressed in the Securities Act and will be governed by the
final adjudication of such issue.
The
undersigned Registrant hereby undertakes that:
|
(1)
|
For
purposes of determining any liability under the Securities Act, the
information omitted from a form of prospectus filed as part of this
registration statement in reliance upon Rule 430A and contained in
the
form of prospectus filed by the Registrant pursuant to Rule 424(b)(1)
or
(4) or 497(h) under the Securities Act shall be deemed to be part
of this
registration statement as of the time it was declared effective.
|
|
(2)
|
For
the purpose of determining any liability under the Securities Act,
each
post-effective amendment that contains a form of prospectus shall
be
deemed to be a new registration statement relating to the securities
offered therein, and the offering of such securities at that time
shall be
deemed to be the initial bona fide offering thereof.
|
|
(3)
|
The
undersigned Registrant hereby undertakes to provide to the underwriter
at
the closing specified in the underwriting agreements, certificates
in such
denominations and registered in such names as required by the underwriter
to permit prompt delivery to each
purchaser.
|
SIGNATURES
Pursuant
to the requirements of the Securities Act of 1933, the registrant certifies
that
it has reasonable grounds to believe that it meets all of the requirements
for
filing on Form F-1 and has duly caused and authorized this registration
statement to be signed on its behalf by the undersigned, thereunto duly
authorized, in the city of New
York,
New
York on April 20, 2006.
|
XTL
BIOPHARMACEUTICALS LTD.
|
||
| |
|
|
| By: | /s/ Ron Bentsur | |
| Ron Bentsur | ||
| Chief Executive Officer | ||
POWER
OF ATTORNEY
KNOW
ALL
MEN BY THESE PRESENTS, that we, the undersigned officers and directors of XTL
Biopharmaceuticals Ltd. hereby severally constitute Ron Bentsur and Jonathan
Burgin, and each of them singly, our true and lawful attorneys with full power
to them, and each of them singly, to sign for us and in our names in the
capacities indicated below, the Registration Statement filed herewith and any
and all amendments to said Registration Statement, including any registration
statements filed pursuant to Rule 462(b), and generally to do all such things
in
our names and in our capacities as officers and directors to enable XTL
Biopharmaceuticals Ltd. to comply with the provisions of the Securities Act
of
1933, as amended, and all requirements of the Securities and Exchange
Commission, hereby ratifying and confirming our signature as they may signed
by
our said attorneys, or any of them, to said Registration Statement and any
and
all amendments thereto.
Pursuant
to the requirements of the Securities Act of 1933, as amended, this Registration
Statement has been signed by the following persons in the capacities indicated
as of April 20, 2006.
|
Signatures
|
Title
|
|
|
/s/
Michael S. Weiss
|
||
|
Michael
S. Weiss
|
Chairman
of the Board of Directors
|
|
|
/s/
Ron Bentsur
|
||
|
Ron
Bentsur
|
Chief
Executive Officer
|
|
|
/s/
Jonathan Burgin
|
||
|
Jonathan
Burgin
|
Chief
Financial Officer and
Chief
Accounting Officer
|
|
|
/s/
William J. Kennedy
|
||
|
William
J. Kennedy
|
Non-executive
Director
|
|
|
/s/
Ido Seltenreich
|
||
|
Ido
Seltenreich
|
Non-executive
Director and External Director
|
|
|
/s/
Vered Shany
|
||
|
Vered
Shany, D.M.D.
|
Non-executive
Director and External Director
|
|
|
/s/
Jonathan R. Spicehandler
|
||
|
Jonathan
R. Spicehandler, M.D.
|
Non-executive
Director
|
|
|
Ben
Zion Weiner, Ph.D
|
Non-executive
Director
|
II-5