Prospective Grant of Exclusive License: GLP-1 Exendin-4 Peptide Analogs and Uses Thereof, 32364 [E6-8678]
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32364
Federal Register / Vol. 71, No. 107 / Monday, June 5, 2006 / Notices
Inventors: Dan A. Buzatu (FDA), Jon
G. Wilkes (FDA), Dwight W. Miller
(FDA), Jerry A. Darsey (Univ Arkansas),
Thomas M. Heinze (FDA), Alexandru S.
Biris (Univ Arkansas), Richard Beger
(FDA).
Patent Status: U.S. Patent Application
No. 11/005,412 filed December 6, 2004
(HHS Reference No. E–090–2004/0-US–
01).
Licensing Status: All licensing
inquiries should be directed to Michael
McAllister, University of Arkansas at
Little Rock, Office of Technology
Transfer, 2801 South University
Avenue, Little Rock, AR 72204–1099;
Phone: 501/569–8658; E-mail:
Jmmccalliste@uaur.edu.
NIH Contact: Michael A. Shmilovich,
Esq.; 301/435–5019;
shmilovm@mail.nih.gov.
Dated: May 24, 2006.
David R. Sadowski,
Acting Director, Division of Technology
Development and Transfer, Office of
Technology Transfer, National Institutes of
Health.
[FR Doc. 06–5105 Filed 6–2–06; 8:45 am]
BILLING CODE 4140–01–P
DEPARTMENT OF HEALTH AND
HUMAN SERVICES
National Institutes of Health
Prospective Grant of Exclusive
License: GLP-1 Exendin-4 Peptide
Analogs and Uses Thereof
National Institutes of Health,
Public Health Service, HHS.
ACTION: Notice.
AGENCY:
This is notice, in accordance
with 35 U.S.C. 209(c)(1) and 37 CFR
404.7(a)(1)(i), that the National
Institutes of Health (NIH), Department
of Health and Human Services, is
contemplating the grant of an exclusive
license worldwide to practice the
invention embodied in U.S. Patent
Application Number 10/485,140 filed
January 27, 2004, entitled ‘‘GLP-1
Exendrin-4 Peptide Analogs and Uses
Thereof,’’ to Amylin Pharmaceuticals,
Inc., having a place of business in San
Diego, CA 92121. The contemplated
exclusive license may be limited to use
to human therapeutics for diabetes,
obesity and cardiovascular disease, as
well as neurological and
neurodegenerative diseases, disorders
and injuries. The United States of
America is the assignee of the patent
rights in this invention.
DATES: Only written comments and/or
application for a license which is
received by the NIH Office of
cprice-sewell on PROD1PC66 with NOTICES
SUMMARY:
VerDate Aug<31>2005
15:33 Jun 02, 2006
Jkt 208001
Technology Transfer on or before
August 4, 2006 will be considered.
Request for a copy of the
patent, inquires, comments, and other
materials relating to the contemplated
license should be directed to: Marlene
Astor, Technology Licensing Specialist,
Office of Technology Transfer, National
Institutes of Health, 6011 Executive
Boulevard, Suite 325, Rockville, MD
20852–3804; Telephone: 301–435–4426;
Facsimile: 301–402–0220; e-mail:
ms482m@nih.gov.
ADDRESSES:
Type-2
diabetes and neurodegeneration (e.g.,
Alzheimer’s disease, Parkinson’s
disease, peripheral neuropathy, stroke)
are leading causes of death in the
United States and worldwide. The
present invention pertains to the
disclosure of novel peptide analogues of
Glucagons-like peptide-1 (GLP-1) and
Exendin-4 and their uses in the
treatment of (i) diabetes and (ii)
neurodegenerative disorders.
Type-2 diabetes is caused by
dysfunction of the pancreatic beta cells
that may result in concomitant decrease
in insulin production. Insulin
replacement has been an effective
therapy for the treatment of Type-2
diabetes. However, insulin therapy,
although life saving, does not restore
normal levels of glucose and
postprandial levels of glucose continues
to be excessively high in individuals on
insulin therapy. Further, the therapy
may result in adverse effects including
hyperglycemia, hypoglycemia,
metabolic acidosis and ketosis.
Therefore, a better therapeutic formula
may be needed that may increase the
efficacy of the treatment and minimize
the side effects. The present invention
discloses a method of treating a subject
with diabetes with novel GLP-1/
Exendin-4 peptides. These are GLP-1
agonists and elicit insulinotropic
actions.
The GLP-1 receptor is additionally
found in the brain as well as associated
to pancreatic islets cells. Its stimulation
in brain has been found to be
neurotrophic and neuroprotective in
both tissue culture and in vivo against
a variety of toxic insults. Peptides of the
said invention possess activity in a
variety of predictive models of
neurodegeneration, and may have
potential in a variety of diseases both
associated (peripheral neuropathy) and
unassociated (Alzheimer’s disease,
Parkinson’s disease, stroke and
peripheral neuropathy) with diabetes J.
Alz. Dis. 4: 487–96, 2002; J. Pharmacol.
Exp. Ther. 300:958–66, 2002 & 302:881–
888, 2002.
SUPPLEMENTARY INFORMATION:
PO 00000
Frm 00064
Fmt 4703
Sfmt 4703
The prospective exclusive license will
be royalty-bearing and will comply with
the terms and conditions of 35 U.S.C.
209 and 37 CFR 404.7. The prospective
exclusive license may be granted unless,
within 60 days from the date of this
published Notice, the NIH receives
written evidence and argument that
establishes that the grant of the license
would not be consistent with the
requirements of 35 U.S.C. 209 and 37
CFR 404.7.
Properly filed competing applications
for a license filed in response to this
notice will be treated as objections to
the contemplated license. Comments
and objections submitted in response to
this notice will not be made available
for public inspection, and, to the extent
permitted by law, will not be released
under the Freedom of Information Act,
5 U.S.C. 552.
Dated: May 26, 2006.
David R. Sadowski,
Acting Director, Division of Technology
Development and Transfer, Office of
Technology Transfer, National Institutes of
Health.
[FR Doc. E6–8678 Filed 6–2–06; 8:45 am]
BILLING CODE 4140–01–P
DEPARTMENT OF HEALTH AND
HUMAN SERVICES
National Institutes of Health
Prospective Grant of Co-Exclusive
License: Human Monoclonal Antibody,
Their Fragments and Derivatives as
Biotherapeutics for the Treatment of
HIV Infections
National Institutes of Health,
Public Health Service, HHS.
ACTION: Notice.
AGENCY:
SUMMARY: This is notice, in accordance
with 35 U.S.C. 209(c)(1) and 37 CFR
404.7(a)(1)(i), that the National
Institutes of Health (NIH), Department
of Health and Human Services, is
contemplating the grant of a coexclusive license to practice the
inventions embodied in:
1. U.S. Provisional Patent Application
Serial No. S/N 60/378,406, PCT/US03/
14905, NIH (DHHS) Ref. No. E–144–
2002/1–PCT–02 converted into
03733940.5 (E–144–2002/1–EP–04) filed
in Europe on November 25, 2004, and
2003239356 (E–144–2002/1–AU–05)
filed in Australia October 29, 2004, 10/
512,966 (E–144–2002/1–US–03) filed in
USA October 28, 2004, as well as
2485120 (E–144–2002/1–CA–06) filed in
Canada May 6, 2003, entitled:
‘‘Identification of Novel Broadly CrossReactive Neutralizing Human
E:\FR\FM\05JNN1.SGM
05JNN1
]]>Agencies
[Federal Register Volume 71, Number 107 (Monday, June 5, 2006)]
[Notices]
[Page 32364]
From the Federal Register Online via the Government Printing Office [www.gpo.gov]
[FR Doc No: E6-8678]
-----------------------------------------------------------------------
DEPARTMENT OF HEALTH AND HUMAN SERVICES
National Institutes of Health
Prospective Grant of Exclusive License: GLP-1 Exendin-4 Peptide
Analogs and Uses Thereof
AGENCY: National Institutes of Health, Public Health Service, HHS.
ACTION: Notice.
-----------------------------------------------------------------------
SUMMARY: This is notice, in accordance with 35 U.S.C. 209(c)(1) and 37
CFR 404.7(a)(1)(i), that the National Institutes of Health (NIH),
Department of Health and Human Services, is contemplating the grant of
an exclusive license worldwide to practice the invention embodied in
U.S. Patent Application Number 10/485,140 filed January 27, 2004,
entitled ``GLP-1 Exendrin-4 Peptide Analogs and Uses Thereof,'' to
Amylin Pharmaceuticals, Inc., having a place of business in San Diego,
CA 92121. The contemplated exclusive license may be limited to use to
human therapeutics for diabetes, obesity and cardiovascular disease, as
well as neurological and neurodegenerative diseases, disorders and
injuries. The United States of America is the assignee of the patent
rights in this invention.
DATES: Only written comments and/or application for a license which is
received by the NIH Office of Technology Transfer on or before August
4, 2006 will be considered.
ADDRESSES: Request for a copy of the patent, inquires, comments, and
other materials relating to the contemplated license should be directed
to: Marlene Astor, Technology Licensing Specialist, Office of
Technology Transfer, National Institutes of Health, 6011 Executive
Boulevard, Suite 325, Rockville, MD 20852-3804; Telephone: 301-435-
4426; Facsimile: 301-402-0220; e-mail: ms482m@nih.gov.
SUPPLEMENTARY INFORMATION: Type-2 diabetes and neurodegeneration (e.g.,
Alzheimer's disease, Parkinson's disease, peripheral neuropathy,
stroke) are leading causes of death in the United States and worldwide.
The present invention pertains to the disclosure of novel peptide
analogues of Glucagons-like peptide-1 (GLP-1) and Exendin-4 and their
uses in the treatment of (i) diabetes and (ii) neurodegenerative
disorders.
Type-2 diabetes is caused by dysfunction of the pancreatic beta
cells that may result in concomitant decrease in insulin production.
Insulin replacement has been an effective therapy for the treatment of
Type-2 diabetes. However, insulin therapy, although life saving, does
not restore normal levels of glucose and postprandial levels of glucose
continues to be excessively high in individuals on insulin therapy.
Further, the therapy may result in adverse effects including
hyperglycemia, hypoglycemia, metabolic acidosis and ketosis. Therefore,
a better therapeutic formula may be needed that may increase the
efficacy of the treatment and minimize the side effects. The present
invention discloses a method of treating a subject with diabetes with
novel GLP-1/Exendin-4 peptides. These are GLP-1 agonists and elicit
insulinotropic actions.
The GLP-1 receptor is additionally found in the brain as well as
associated to pancreatic islets cells. Its stimulation in brain has
been found to be neurotrophic and neuroprotective in both tissue
culture and in vivo against a variety of toxic insults. Peptides of the
said invention possess activity in a variety of predictive models of
neurodegeneration, and may have potential in a variety of diseases both
associated (peripheral neuropathy) and unassociated (Alzheimer's
disease, Parkinson's disease, stroke and peripheral neuropathy) with
diabetes J. Alz. Dis. 4: 487-96, 2002; J. Pharmacol. Exp. Ther.
300:958-66, 2002 & 302:881-888, 2002.
The prospective exclusive license will be royalty-bearing and will
comply with the terms and conditions of 35 U.S.C. 209 and 37 CFR 404.7.
The prospective exclusive license may be granted unless, within 60 days
from the date of this published Notice, the NIH receives written
evidence and argument that establishes that the grant of the license
would not be consistent with the requirements of 35 U.S.C. 209 and 37
CFR 404.7.
Properly filed competing applications for a license filed in
response to this notice will be treated as objections to the
contemplated license. Comments and objections submitted in response to
this notice will not be made available for public inspection, and, to
the extent permitted by law, will not be released under the Freedom of
Information Act, 5 U.S.C. 552.
Dated: May 26, 2006.
David R. Sadowski,
Acting Director, Division of Technology Development and Transfer,
Office of Technology Transfer, National Institutes of Health.
[FR Doc. E6-8678 Filed 6-2-06; 8:45 am]
BILLING CODE 4140-01-P
