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8-K - FORM 8-K - HUMAN GENOME SCIENCES INC | c26460e8vk.htm |
EX-99.2 - EXHIBIT 99.2 - HUMAN GENOME SCIENCES INC | c26460exv99w2.htm |
Exhibit 99.1
PRESS RELEASE
Media Contacts:
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Investor Contacts: | |
Susannah Budington
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Claudine Prowse, Ph.D. | |
Director, Corporate Public Relations
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Executive Director, Investor Relations | |
301-545-1062
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301-315-1785 | |
Jerry Parrott
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Peter Vozzo | |
Vice President, Corporate Communications
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Senior Director, Investor Relations | |
301-315-2777
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301-251-6003 |
HUMAN GENOME SCIENCES REPORTS PROGRESS WITH COMMERCIALIZATION OF BENLYSTA® AND ANNOUNCES
2012 GOALS AT JPMORGAN HEALTHCARE CONFERENCE
| 2011 BENLYSTA® gross sales $59.2 million; net sales $52.3 million | ||
| Steady progress toward broader adoption of BENLYSTA treatment |
ROCKVILLE, Maryland January 9, 2012 Human Genome Sciences, Inc. (Nasdaq: HGSI) will today
announce its priority goals for 2012 and report on progress with the commercialization of BENLYSTA®
(belimumab), the first approved drug for systemic lupus in 56 years, during a presentation this
afternoon by H. Thomas Watkins, President and Chief Executive Officer, to financial analysts and
investors at the 30th Annual JPMorgan Healthcare Conference in San Francisco.
Thousands of patients with systemic lupus are now being treated with BENLYSTA, said Mr. Watkins.
We are pioneering a treatment in a market that has not seen a new option for patients in decades.
Although we are still in the early adoption phase of our launch, our experience in the market to
date reinforces our belief that BENLYSTA will ultimately play a major role in improving the
standard of care for SLE patients.
During his presentation, Mr. Watkins will discuss the following goals and updates on progress:
BENLYSTA® FOR SLE: APPROVED BY FDA IN MARCH 2011, BY CANADA AND EUROPEAN COMMISSION IN JULY 2011,
AND NOW BECOMING AVAILABLE TO INCREASING NUMBERS OF PATIENTS AROUND THE WORLD
BENLYSTA (belimumab) was approved on March 9, 2011 by the U.S. Food and Drug Administration (FDA)
for the treatment of adult patients with active, autoantibody-positive systemic lupus erythematosus
(SLE) who are receiving standard therapy.
Estimated BENLYSTA gross sales totaled $29.1 million in the fourth quarter of 2011. After
gross-to-net adjustments of $3.4 million, estimated net sales of BENLYSTA in the fourth quarter
totaled $25.7 million. During the fourth quarter, estimated BENLYSTA average weekly gross sales
for the first four weeks were $2.3 million, followed by average
weekly gross sales of $2.1 million and $2.5 million for the
second and third four-week periods, respectively.
Estimated BENLYSTA gross sales for the year ended December 31, 2011, reflecting three full quarters
on the market, totaled $59.2 million. After gross-to-net
adjustments of $6.9 million, estimated net sales of BENLYSTA for 2011 totaled $52.3 million.
With BENLYSTA, we are working to change the paradigm of treatment for systemic lupus, said
Mr. Watkins. This involves significant education on clinical data that are still unfamiliar to
many lupus-treating physicians, followed by physicians initial trial of BENLYSTA in a few of their
real world patients. We have seen good progress with the number of physicians initiating use. As
they build their own clinical experience, more and more physicians are considering BENLYSTA for
appropriate SLE patients. We believe that BENLYSTA is on its way to becoming an important
component of a new standard of care for SLE.
HGS sales data suggest that more than 40% of key accounts have initiated treatment with BENLYSTA as
of the end of December 2011, compared with approximately 30% at the end of the third quarter.
Among the community-based accounts that are the largest infusing practices, approximately 50% have
begun to purchase BENLYSTA. Among key hospital accounts, which are hospitals with very large lupus
cohorts, more than 40% have begun to purchase BENLYSTA. In market research, more than half of
rheumatologists report that they have begun to prescribe BENLYSTA for SLE patients; this is an
encouraging leading indicator for further increases in purchasing accounts.
BENLYSTA was approved by the European Commission on July 13, 2011, and is now available in Canada
and an increasing number of European countries, including Germany, Spain, Austria, Denmark,
Finland, Hungary, Norway and Sweden. HGS has built its own commercialization team to work alongside
GSK in Europe, with headquarters in Switzerland and local organizations in Germany, France and
Spain.
Elsewhere, GSK leads local implementation, with HGS sharing costs and profits equally with GSK.
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In December 2011, HGS and GSK announced that the dosing of patients has been initiated in BLISS-SC,
a Phase 3 trial of the subcutaneous formulation of BENLYSTA. Assuming that this trial is
successful and regulatory authorities agree, the subcutaneous formulation would make it possible
for patients to self-administer BENLYSTA by injection once a week. In May 2011, GSK initiated
dosing in the BENLYSTA Phase 3 trial in East Asia, which will enroll approximately 630 patients in
China, Japan and South Korea.
Key goals for BENLYSTA in 2012:
| Continue to increase sales in the U.S. and elsewhere. | ||
| Continue to work with GSK to launch BENLYSTA in countries around the world. | ||
| Enroll Phase 3 trial of subcutaneous formulation throughout 2012; complete enrollment in 2013. | ||
| Initiate Phase 3 trial in vasculitis. | ||
| Initiate Phase 3 trial in active lupus nephritis. | ||
| Enroll Phase 3 trial in East Asia. |
RAXIBACUMAB: DELIVERIES TO U.S. STRATEGIC NATIONAL STOCKPILE CONTINUE
HGS continues to deliver raxibacumab to the U.S. Strategic National Stockpile for emergency use in
treating inhalation anthrax. Raxibacumab is being developed under a contract entered into in 2006
with the Biomedical Advanced Research and Development Authority (BARDA) of the Office of the
Assistant Secretary for Preparedness and Response (ASPR), U.S. Department of Health and Human
Services (HHS). In July 2009, the U.S. Government exercised its option to purchase an additional
45,000 doses of raxibacumab, with delivery to be completed over a three-year period. HGS expects
to receive approximately $142 million from this second award as deliveries are completed, including
approximately $52.5 million recognized in 2011. HGS also continues to work closely with FDA to
achieve licensure of raxibacumab, and is entitled to receive $20 million under its contract with
the U.S. Government upon FDA licensure.
Key goals for raxibacumab in 2012:
| Deliver approximately 8,000 doses to the U.S. Strategic National Stockpile and receive approximately $25 million in revenue as deliveries are accepted. | ||
| Continue to work with the FDA to achieve licensure of raxibacumab. |
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GSK PIPELINE: INITIAL RESULTS OF PHASE 3 TRIALS OF ALBIGLUTIDE FOR TYPE 2 DIABETES EXPECTED
MID-2012; ENROLLMENT COMPLETED IN SECOND PHASE 3 TRIAL OF DARAPLADIB FOR CARDIOVASCULAR DISEASE
GSKs Phase 3 program to evaluate the long-term efficacy, safety and tolerability of albiglutide as
monotherapy and add-on therapy for patients with type 2 diabetes mellitus continues to move
forward. GSK announced topline results of the first of eight Phase 3 trials in November 2011. The
study, known as Harmony 7, was designed to compare once-weekly albiglutide to once-a-day
liraglutide. Results showed a reduction in HbA1c from baseline of 0.78% for patients receiving
albiglutide compared to a reduction of 0.99% for liraglutide. Although the pre-specified margin of
non-inferiority to liraglutide was not met, albiglutide did show a statistically significant
reduction in HbA1c from baseline (p<0.001). The most common adverse events observed during this
study were nausea (9.9% for abiglutide versus 29.2% for liraglutide) and vomiting (5%for abiglutide
versus 9.3% for liraglutide).
GSKs conclusion after review of the data is that the data support continued progress toward
registration as a possible once-weekly treatment for type 2 diabetes. GSK expects initial results
from the remaining studies over the course of the next several months, and has stated that it
expects to provide an update on albiglutide once a more complete view of the data is available in
mid-2012. Albiglutide was created by HGS using its proprietary albumin-fusion technology, and the
product was licensed to GSK in 2004. HGS is entitled to fees and milestone payments that could
amount to as much as $183 million including $33 million received to date in addition to
single-digit royalties on worldwide sales if albiglutide is commercialized.
GSKs Phase 3 program for darapladib is also progressing and is evaluating whether darapladib can
reduce the risk of adverse cardiovascular events such as heart attack or stroke in patients with
chronic coronary heart disease (CHD) and acute coronary syndrome (ACS), respectively. In October
2011, GSK completed the enrollment of over 13,000 patients into the SOLID-TIMI 52 study of
darapladib in patients who have suffered an ACS event. The SOLID-TIMI 52 study is one of two
pivotal Phase 3 trials in the darapladib clinical program. The other study is STABILITY, which is
evaluating darapladib in patients with CHD and in 2010 completed the enrollment of about 15,800
patients. The combined program spans 42 countries and has enrolled more than 28,500 patients at
more than 1500 clinical sites. Darapladib was discovered by GSK based on HGS technology. HGS will
receive 10% royalties on worldwide sales if darapladib is commercialized, and has a 20%
co-promotion option in North America and Europe.
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MID- AND EARLY-STAGE PIPELINE
A randomized Phase 2 trial is currently evaluating mapatumumab in combination with Nexavar
(sorafenib) for the treatment of advanced hepatocellular cancer. Mapatumumab is a human monoclonal
antibody to TRAIL receptor 1.
In March 2011, HGS and FivePrime Therapeutics announced a collaboration to develop and
commercialize HGS1036 (formerly FP-1039) for multiple cancers. HGS1036 is a first-in-class
biologic discovered by FivePrime that targets multiple fibroblast growth factor (FGF) ligands. FGF
proteins are growth factors that play important roles in the growth and survival of a number of
solid tumors. A Phase 1 study was completed in 2011, showing that HGS1036 was safe and well
tolerated. In 2012, HGS plans to initiate Phase 1b trials of HGS1036 in combination with
chemotherapy.
HGS has halted development of two early-stage products: HGS1029, an IAP inhibitor in Phase 1
development in patients with advanced solid and advanced lymphoid tumors, and HGS1025, a human
monoclonal antibody to the CCR5 receptor that would have entered Phase 1b development in ulcerative
colitis.
Key goals for the HGS mid- and early-stage pipeline in 2012 are:
| Complete enrollment of the randomized Phase 2 trial of mapatumumab with sorafenib in advanced hepatocellular cancer. | ||
| Initiate Phase 1b oncology studies of HGS1036 in combination with chemotherapy agents. |
ORGANIZATIONAL DOWN-SIZING REFLECTS CONTINUED COMMITMENT TO MORE EFFICIENT OPERATIONS
HGS today announced that it is eliminating approximately 150 positions and reducing spending to
reflect current program and business requirements. Positions across the company were affected,
including manufacturing, R&D and administration.
We will continue to make the investments required for the successful worldwide commercialization
of BENLYSTA, said Mr. Watkins. We remain committed to achieving profitability in 2014 and
sustainable revenues into the future.
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FINANCIAL GUIDANCE
During his presentation to the 30th annual JPMorgan Healthcare Conference, Mr. Watkins
will present the following guidance regarding financial results expected by HGS for the full years
2011 and 2012.
| HGS expects cash and investments at year-end 2011 to total between approximately $875 million and $885 million, compared with $933.4 million at year-end 2010. This includes approximately $430 million in net cash from the Companys successful public offering of Convertible Senior Notes completed in November 2011. | |
| HGS expects key expenses to total in the following ranges: |
| R&D expense is expected to total between approximately $195 million and $205 million in 2011, and between approximately $150 million and $180 million in 2012. | ||
| SG&A expense is expected to total between approximately $155 million and $165 million in 2011, and between approximately $160 million and $180 million in 2012. |
PRESENTATION TO BE WEBCAST
Mr. Watkins presentation to the 30th Annual JPMorgan Healthcare Conference will be
webcast and may be accessed at www.hgsi.com. The presentation is scheduled to begin on January 9,
2012, at 4:30 PM Pacific or 7:30 PM Eastern time. Investors interested in listening to the live
webcast may want to log on before the presentation begins to download any software required. The
archive of the presentation will be available for several days following the event.
ABOUT HUMAN GENOME SCIENCES
Human Genome Sciences exists to place new therapies into the hands of those battling serious
disease.
For more information about HGS, please visit the Companys web site at www.hgsi.com. Health
professionals and patients interested in clinical trials of HGS products may inquire via email to
clinicaltrialsinfo@hgsi.com or by calling HGS at 1-240-314-4430.
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HGS, Human Genome Sciences and BENLYSTA are trademarks of Human Genome Sciences, Inc. Other
trademarks referenced are the property of their respective owners.
SAFE HARBOR STATEMENT
This announcement includes statements that are forward-looking within the meaning of the Private
Securities Litigation Reform Act of 1995. These forward-looking statements include those regarding
our expectations for BENLYSTA, business goals for 2012 and financial guidance, among others. These
forward-looking statements are based on our current intentions, beliefs and expectations regarding
future events. We cannot guarantee that any forward-looking statement will be accurate. Investors
should realize that if underlying assumptions prove inaccurate or unknown risks or uncertainties
materialize, actual results could differ materially from our expectations. Investors are,
therefore, cautioned not to place undue reliance on any forward-looking statement. Any
forward-looking statement speaks only as of the date of this announcement, and, except as required
by law, we do not undertake to update any forward-looking statement to reflect new information,
events or circumstances.
Some important factors that could cause our actual results to differ from our expectations in these
forward-looking statements include: our lack of commercial experience and dependence on the sales
growth of BENLYSTA; any failure to commercialize BENLYSTA successfully; the occurrence of adverse
safety events with our products; changes in the availability of reimbursement for BENLYSTA; the
inherent uncertainty of the timing, success of, and expense associated with, research, development,
regulatory approval and commercialization of our pipeline products and new indications for existing
products; substantial competition in our industry, including from branded and generic products; the
highly regulated nature of our business; uncertainty regarding our intellectual property rights and
those of others; the ability to manufacture at appropriate scale, and in compliance with regulatory
requirements, to meet market demand for our products; our substantial indebtedness and lease
obligations; our dependence on collaborations over which we may not always have full control;
foreign exchange rate valuations and fluctuations; the impact of our acquisitions and strategic
transactions; changes in the health care industry in the U.S. and other countries, including
government laws and regulations relating to sales and promotion, reimbursement and pricing
generally; significant litigation adverse to the Company, including product liability and patent
infringement claims; our ability to attract and retain key personnel; and increased scrutiny of the
health care industry by government agencies and state attorneys general resulting in investigations
and prosecutions.
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The foregoing list sets forth many, but not all, of the factors that could cause actual results to
differ from our expectations in any forward-looking statement. Investors should consider this
cautionary statement, as well as the risk factors identified in our periodic reports filed with the
SEC, when evaluating our forward-looking statements.
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