Full Press Release Details
OncoGenex Reports Financial Results for Fourth Quarter and Fiscal Year 2009
and Provides Outlook for 2010
Conference Call on Monday, March 8, 2010 at 4:30 p.m. Eastern Time
BOTHELL, WA, and VANCOUVER, March 8, 2010 OncoGenex Pharmaceuticals, Inc. ( OncoGenex or the
Company ) (NASDAQ: OGXI), today announced its fourth quarter and fiscal year 2009 financial
results, reviewed the Company s highlights and provided an outlook for 2010.
2009 was a transformative year for OncoGenex culminating in the signing of a collaboration
agreement with Teva for the development of OGX-011 which includes initiating three Phase III
clinical studies, said Scott Cormack, President and Chief Executive Officer of OncoGenex. At the
2009 ASCO Annual General Meeting we announced that our Phase II study in patients with advanced
prostate cancer who received OGX-011 in combination with first-line chemotherapy had a 6.9 month
median survival advantage compared to first-line chemotherapy alone. To date we have treated almost
300 patients with OGX-011 over the course of various clinical trials including five Phase II
clinical studies in patients with prostate, lung, and breast cancer. We start 2010 with a stronger
cash position, a stronger clinical data package, a clear path for Phase III development, and a
development partner that has committed capital resources to drive our joint development plan. We
look forward to a productive 2010 as we initiate our Phase III development plan for OGX-011 and
continue to advance OGX-427 into Phase II development.
Revenue for the fourth quarter and full year of 2009 was $25.5 million, consisting of partial
recognition of the non-refundable up-front payments received from Teva in December 2009. Previously
we had not recognized any revenue. At December 31, 2009, $26.5 million of the upfront payment was
included in the Company s Balance Sheet as Deferred Collaboration Revenue which we are amortizing
over a period of approximately three years based on the expected performance period of our
deliverables under this agreement.
Research and development expenses for the fourth quarter and year ended December 31, 2009 were
$17.4 million and $24.2 million, respectively, compared to $4.2 million and $7.8 million,
respectively, in the corresponding periods of 2008. The increases in 2009 were due mainly to
amounts owing pursuant to our licensing agreements with Isis Pharmaceuticals ( Isis ) and the
University of British Columbia ( UBC ) in connection with the upfront payments we received in our
global license and collaboration agreement ( Collaboration Agreement ) with Teva Pharmaceuticals
Industries Ltd. ( Teva ) in the fourth quarter of 2009, higher OGX-011 and OGX-427 development
costs, increases in employee expenses and higher facility costs resulting from the reverse takeover
of Sonus Pharmaceuticals, Inc. ( Sonus ).
General and administrative expenses for the fourth quarter and year ended December 31, 2009 were
$1.3 million and $4.0 million, respectively, compared to $1.0 million and $3.3 million, respectively, in the corresponding periods of 2008. The increase for the year ended
December 31, 2009 was primarily due to higher employee expenses and increased costs associated with
operating as a public company in 2009. The increase in costs for the fourth quarter of 2009,
compared to the same quarter of 2008 was primarily due to higher employee expenses and expenses
incurred in connection with closing our Collaboration Agreement with Teva.
The Company realized net income for the fourth quarter of 2009 of $3.9 million compared to a net
loss of $5.0 million in the corresponding period of 2008. On an annual basis net loss decreased
from $6.2 million in 2008 to $5.5 million in 2009. The decreased loss in 2009 as compared to 2008
on both an annual and quarterly basis, was primarily due to revenue recognized in connection with
the Collaboration Agreement with Teva, offset by milestone payments made to Isis and UBC and higher
research and development costs initiated in the fourth quarter of 2009 that were associated with
critical path activities for the planned Phase III trials of OGX-011. In 2009 an income tax expense
of $3.0 million was the result of potential withholding taxes payable to the Israel Tax Authority
in connection with our Collaboration Agreement with Teva. In 2008 the income tax recovery of $2.1
million was primarily the result of a reversal of tax expense associated with the change in capital
structure of OncoGenex Technologies, a non-cash item. The Company had $64.6 million in cash, cash
equivalents and short-term investments as of December 31, 2009, compared to $12.4 million as of
December 31, 2008. The increase in cash, cash equivalents and short-term investments in 2009 as
compared to 2008 was due to the upfront payment received from Teva as part of the Collaboration
Agreement in December 2009.
In the first quarter of 2010 we paid Isis and UBC a total of $10.3 million for the license expenses
accrued in the fourth quarter of 2009. For 2010, we anticipate that we will incur operating
expenses of between $21 million and $23 million and anticipate ending the year with cash, cash
equivalents, and short-term investments of between $29 million and $31 million, respectively. We
believe we have sufficient cash, cash equivalents and short-term investments to fund currently
planned operations into 2012 and expect that both Phase III prostate cancer trials will be fully
accrued by this time. The Company had 6,333,685 shares outstanding as at March 8, 2010.
The consolidated results discussed above reflect the operations of OncoGenex Technologies Inc.
( OncoGenex Technologies ) prior to the August 21, 2008 reverse takeover of Sonus, and the
consolidated results of the OncoGenex Pharmaceuticals thereafter.
| In collaboration with Teva, initiate a Phase III trial evaluating OGX-011 with docetaxel retreatment as second-line therapy in castrate resistant prostate cancer ( CRPC ) in the second quarter of 2010 subject to institutional review board approvals and patient screening | |||
| In collaboration with Teva, initiate a Phase III trial evaluating OGX-011 with first-line docetaxel treatment in CRPC in the third quarter of 2010 | |||
| In collaboration with Teva, continue critical path initiatives including manufacturing readiness and clinical trial design for a Phase III trial evaluating OGX-011 with first-line chemotherapy in Non-Small Cell Lung Cancer ( NSCLC ) to be initiated in early 2011 |
| Complete accrual of OGX-427 Phase I trial in solid tumors (evaluating OGX-011 as monotherapy and in combination with docetaxel) | |||
| Report final data from OGX-427 Phase I trial in solid tumors | |||
| Initiate an investigator-sponsored, randomized, controlled Phase II trial evaluating OGX-427 as a monotherapy in prostate cancer |
In December 2009, OncoGenex entered into the Collaboration Agreement with Teva to develop and
commercialize OGX-011. OGX-011 is expected to be used as adjunct therapy to enhance the
effectiveness of chemotherapy and has shown promising results when added to currently available
chemotherapies in several tumor types addressing a significant unmet medical need. Teva and
OncoGenex will collaborate on a global Phase III clinical program, with two Phase III clinical
trials expected to be initiated in 2010: a Phase III study for second-line chemotherapy in men with
CRPC and a Phase III study in first-line chemotherapy for men with CRPC. An additional Phase III
study in first-line treatment of advanced, unresectable NSCLC is intended to be initiated by early
In February 2010, OncoGenex received written, scientific advice from the European Medicines Agency
(EMA) on the company s development plan for OGX-011 for the treatment of men with CRPC. The input
received from the Committee for Medicinal Products for Human Use (CHMP) at the EMA was generally in
agreement with OncoGenex s development plan regarding the proposed preclinical studies and both the
study designs and analyses for the Phase III trials in CRPC. The CHMP also agreed that the intended
safety database would enable a sufficiently qualified risk-benefit assessment for market approval.
OncoGenex Pharmaceuticals had previously announced completion of the following two Special Protocol
Assessment (SPA) agreements with the Food and Drug Administration (FDA) for the two Phase III
trials: the SPA for Study OGX-011-10 that was announced on April 28, 2009 and the SPA for Study
OGX-011-11 that was announced on June 24, 2009.
In January 2010, OncoGenex announced that an investigator-sponsored, randomized, controlled Phase
II clinical trial evaluating OGX-427 when administered as a monotherapy to patients with CRPC
received grant funding. The funds were awarded by a third party granting agency to Dr. Kim Chi, a
medical oncologist at the BC Cancer Agency, Research Scientist at the Vancouver Prostate Centre and
the principal investigator of the OGX-427 Phase II trial.
Conference Call Today at 4:30 p.m. ET
OncoGenex management will host a conference call at 4:30 p.m. Eastern Time today, Monday, March 8,
2010, to provide a business update and discuss the fourth quarter and fiscal year 2009 results. A
live webcast and slide presentation will be available through the Events and Presentations Web page
found in the Investor Relations section of the OncoGenex Web site at www.ir.oncogenex.com.
Alternatively, you may access the live conference call by dialing 877-604-9670 (U.S. Canada) or
719-325-4746 (International). A webcast replay will be available approximately two hours after the call and will
be archived at the same Web location for 90 days.
About OncoGenex Pharmaceuticals
OncoGenex is a biopharmaceutical company committed to the development and commercialization of new
cancer therapies that address treatment resistance in cancer patients. OncoGenex has a deep