Alle Storys
Folgen
Keine Story von Eli Lilly and Company mehr verpassen.

Eli Lilly and Company

Study Demonstrated Once-Weekly Exenatide LAR Improved Glucose Control in Patients with Type 2 Diabetes

Copenhagen, Denmark (ots/PRNewswire)

Eli Lilly and Company (NYSE: LLY), Amylin Pharmaceuticals, Inc.
(Nasdaq: AMLN), and Alkermes, Inc. (Nasdaq: ALKS) today announced
detailed results from a safety and efficacy study of the long-acting
release (LAR) formulation of exenatide. Data from the study
demonstrated that 86 percent of patients using the higher of two
doses of the once-weekly formulation of exenatide were able to
achieve recommended levels of glucose control, as measured by
hemoglobin A1C (HbA1C) with an average improvement of approximately 2
percent compared to placebo. These study findings were presented
today at the Annual Meeting of the European Association for the Study
of Diabetes (EASD) in Copenhagen.
The study was conducted in 45 patients with type 2 diabetes unable
to achieve adequate glucose control with metformin or a diet and
exercise regimen. The patients received a once-weekly subcutaneous
injection of exenatide LAR (either 0.8 mg or 2.0 mg) or placebo.
After 15 weeks of treatment there was a 12-week safety monitoring
period during which no study medication was administered.
Dose-dependent improvements in HbA1C and weight loss were observed
at 15 weeks. At the beginning of the study, the average HbA1C of
study participants was approximately 8.5 percent. In subjects
receiving the 2.0 mg dose of exenatide LAR, the average reduction in
HbA1C was 1.7 percent compared to an increase of 0.4 percent in the
placebo group. Those receiving the 0.8 mg dose improved with an
average decrease in HbA1C of 1.4 percent.
In patients administered 0.8 mg or 2.0 mg of exenatide LAR, 33
percent and 86 percent achieved HbA1C levels of 7 percent or less,
respectively. None of the patients given placebo achieved this target
level of glucose control. HbA1C is a reflection of a person's average
glucose level over approximately three months and is often used by
doctors as a measure of glucose management.
Fasting blood glucose levels were reduced by an average of 39
mg/dL in the 2.0 mg arm and 43 mg/dL in the 0.8 mg arm compared to an
average increase of 18 mg/dL in the placebo group at week 15. Average
fasting blood glucose level at the beginning of the study was 179
mg/dL. Patients who received 2.0 mg of exenatide LAR also experienced
average reductions in body weight of 3.8 kilograms (8.4 pounds) at
week 15 with no evidence of plateau at this point in time; body
weight remained essentially unchanged for the 0.8 mg and placebo
groups. The most frequent adverse event was mild nausea, experienced
by 27 percent of subjects in the 2.0 mg dose group and 19 percent of
subjects in the 0.8 mg dose group compared to 15 percent in the
placebo group. No severe hypoglycemia was observed, and no subjects
receiving either dose of exenatide LAR withdrew because of adverse
events. These detailed findings supplement the preliminary results
released in 2005.
"In this study, the long-acting formulation of exenatide improved
glycemic and weight control and was well tolerated as a combination
therapy with metformin or as stand alone therapy with diet and
exercise," said Michael Trautmann, M.D., Medical Fellow at Eli Lilly
and Company and an author of the study. "These early results suggest
exenatide LAR can be clinically beneficial to patients with type 2
diabetes."
Exenatide LAR uses the proprietary Medisorb(R) drug-delivery
technology developed by Alkermes. The technology encapsulates active
medication into polymer-based microspheres that are injected into the
body, where they degrade slowly -- gradually releasing the drug at a
carefully controlled rate.
Exenatide is the first in a new class of medicines known as
incretin mimetics and was approved for use in the United States by
the U.S. Food and Drug Administration (FDA) in April 2005 for the
treatment of type 2 diabetes. Exenatide is injected twice daily. The
U.S. is the first country in the world that has received regulatory
approval for exenatide. In late 2005, Lilly submitted exenatide for
approval in the European Union. Lilly, Amylin, and Alkermes are
working together to develop a sustained release, subcutaneous
injection of exenatide for the treatment of type 2 diabetes based on
Alkermes' proprietary Medisorb(R) injectable long-acting release drug
delivery technology. Exenatide LAR has not been approved by the FDA
for marketing in the United States.
About exenatide
Exenatide is the first incretin mimetic, a new class of drugs for
the treatment of type 2 diabetes. Exenatide exhibits many of the same
effects as the human incretin hormone glucagon-like peptide-1
(GLP-1). GLP-1, secreted in response to food intake, has multiple
effects on the intestine, liver, pancreas, and brain that work in
concert to regulate blood sugar.(1)
About Incretin Mimetics
Incretin mimetics is a distinct class of treatment in the fight
against diabetes. An incretin mimetic works to mimic the
anti-diabetic or glucose-lowering actions of naturally occurring
human hormones called incretins. These actions include stimulating
the body's ability to produce insulin in response to elevated levels
of blood sugar, inhibiting the release of a hormone called glucagon
following meals, slowing the rate at which nutrients are absorbed
into the bloodstream and reducing food intake. Exenatide is the first
FDA-approved incretin mimetic.
About Diabetes
Diabetes affects an estimated 194 million adults worldwide(2) and
around 48.4 million in Europe.(3) Approximately 90 to 95 percent of
those are affected by type 2 diabetes, a condition characterized by
failure of the pancreatic beta cells to adequately respond to the
increased demands for insulin that occur as a result of
obesity-related insulin resistance.(4) Type 2 diabetes usually occurs
in adults over the age of 40, but is increasingly common in younger
people.(3) In virtually every developed society, diabetes is ranked
among the leading causes of blindness, renal failure and lower limb
amputation, as well as death through its effects on cardiovascular
disease (70-80 percent of people with diabetes die of cardiovascular
disease)(5). The calculated estimates of the costs of diabetes care
in Europe amount to 42.8 million International Dollars per year.(6)
About Lilly, Amylin, and Alkermes
Through a long-standing commitment to diabetes care, Lilly
provides patients with breakthrough treatments that enable them to
live longer, healthier, and fuller lives. Since 1923, Lilly has been
the industry leader in pioneering therapies to help health care
professionals improve the lives of people with diabetes, and research
continues on innovative medicines to address the unmet needs of
patients.
Lilly, a leading innovation-driven corporation is developing a
growing portfolio of first-in-class and best-in-class pharmaceutical
products by applying the latest research from its own worldwide
laboratories and from collaborations with eminent scientific
organizations. Headquartered in Indianapolis, IN, Lilly provides
answers -- through medicines and information -- for some of the
world's most urgent medical needs.
Amylin Pharmaceuticals is a biopharmaceutical company committed to
improving lives through the discovery, development and
commercialization of innovative medicines. Amylin's research and
development activities leverage the company's expertise in metabolism
to develop promising therapies to treat diabetes, obesity and
cardiovascular disease. Amylin is located in San Diego, California
with over 1200 employees nationwide.
Alkermes, Inc. is a biotechnology company that develops products
based on sophisticated drug delivery technologies to enhance
therapeutic outcomes in major diseases. The Company has two
commercial products and a pipeline of extended-release injectable
products and pulmonary products based on its proprietary technology
and expertise. The Company's headquarters are in Cambridge,
Massachusetts, and it operates research and manufacturing facilities
in Massachusetts and Ohio.
This press release contains forward-looking statements, which
involve risks and uncertainties within the meaning of the Private
Securities Litigation Reform Act of 1995. The forward-looking
statements are neither promises nor guarantees, and the businesses of
Lilly, Amylin, and Alkermes are subject to significant risks and
uncertainties. Actual results may differ materially from the
forward-looking statements discussed in this press release. These
forward-looking statements include risks and uncertainties, including
but not limited to, that current or future clinical trials will not
confirm previous results; risks and uncertainties that Amylin will be
able to complete manufacturing scale-up and construction and
validation of its manufacturing facility on a timely basis, or at
all; risks and uncertainties inherent in the collaboration with and
dependence upon Lilly, Amylin and/or Alkermes; risks and
uncertainties regarding the drug discovery and development process,
including whether exenatide LAR will receive regulatory approvals, be
commercialized or prove to be commercially successful. These and
additional risks and uncertainties are described more fully in Lilly,
Amylin, and Alkermes' filings with the United States Securities and
Exchange Commission, including their recently filed Form 10-Qs. The
parties disclaim any obligation to update forward-looking statements.
P-LLY
REFERENCES
(1) Kolterman, O, Buse J, Fineman M, Gaines E, Heintz S, Bicsak T,
Taylor K, Kim D, Aisporna M, Wang Y, Baron A. Synthetic exendin-4
(exenatide) significantly reduces postprandial and fasting glucose in
subjects with type 2 diabetes. Journal of Clinical Endocrinology &
Metabolism. 2003; 88(7):3082-3089.
(2) The International Diabetes Federation Diabetes Atlas.
Available at: http://www.idf.org/home/index.cfm?unode=3B96906B-C026-2
FD3-87B73F80BC22682A. Accessed April 12, 2005.
(3) The International Diabetes Federation, Prevalence / All
diabetes. Available at
http://www.eatlas.idf.org/Prevalence/All_diabetes/.
(4) Turner RC, Cull CA, Frighi V, Holman RR. Glycemic control with
diet, sulfonylurea, metformin, or insulin in patients with type 2
diabetes mellitus: progressive requirement for multiple therapies
(UKPDS 49). JAMA. 1999; 281 (21):2005-2012.
(5) The International Diabetes Federation, Complications.
Available at http://www.eatlas.idf.org/Complications/.
(6) The International Diabetes Federation, Diabetes Atlas, Second
edition. The Economic Impact of Diabetes. 2003: 186.
(Logo: http://www.newscom.com/cgi-bin/prnh/20031219/LLYLOGO
           http://www.newscom.com/cgi-bin/prnh/20060610/AMYLINLOGO
           http://www.newscom.com/cgi-bin/prnh/20050614/ALKSLOGO )

Contact:

Lilly - Derin Denham, +1-317-277-6749 (office), +1-317-370-1435
(cell); Amylin - Alice Bahner, +1-858-642-7272 (office),
+1-858-232-9072 (cell); Alkermes - Rebecca Peterson, +1-617-583-6378
(office), +1-617-899-2447 (cell). Photo: NewsCom:
http://www.newscom.com/cgi-bin/prnh/20031219/LLYLOGO ;
http://www.newscom.com/cgi-bin/prnh/20060610/AMYLINLOGO ;
http://www.newscom.com/cgi-bin/prnh/20050614/ALKSLOGO ; PRN Photo
Desk, photodesk@prnewswire.com

Weitere Storys: Eli Lilly and Company
Weitere Storys: Eli Lilly and Company
  • 20.03.2006 – 13:09

    Lilly and Biosite to Collaborate on Clinical Trial Using Tailored Xigris Therapy

    Indianapolis and San Diego (ots/PRNewswire) - - Trial to Study Use of Biomarker to Better Define Xigris Patients and Treatment Response Eli Lilly and Company (NYSE: LLY) and Biosite(R) Incorporated (Nasdaq: BSTE) today announced the two companies have signed an agreement to collaborate in connection with a clinical trial employing a tailored therapy ...

  • 09.03.2006 – 12:06

    Lilly Launches Phase III Trial of Targeted Cancer Agent

    Indianapolis (ots/PRNewswire) - - Enzastaurin Study Enrolling Patients with Glioblastoma One of the deadliest and rarest forms of cancer is the focus of a Phase III study initiated by Eli Lilly and Company today. Enzastaurin, an investigational, targeted, oral agent, will be evaluated at more than 100 sites worldwide for the treatment of relapsed glioblastoma multiforme (GBM), an aggressive and malignant form ...