Government-Owned Inventions; Availability for Licensing, 16169-16170 [E6-4611]
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Federal Register / Vol. 71, No. 61 / Thursday, March 30, 2006 / Notices
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[FR Doc. 06–3008 Filed 3–29–06; 8:45 am]
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DEPARTMENT OF HEALTH AND
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National Institutes of Health
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Notice of Establishment
Pursuant to the Federal Advisory
Committee Act, as amended (5 U.S.C.
Appendix 2), the Director, National
Institutes of Health (NIH), announces
the establishment of the National Cancer
Institute Clinical Trials Advisory
Committee (Committee).
This Committee shall advise the
Director, NCI, NCI Deputy Directors,
and the Director of each NCI Division on
the NCI-support national clinical trials
enterprise to build a strong scientific
infrastructure by bringing together a
broadly developed and engaged
coalition of stakeholders involved in the
clinical trials process.
The Committee will consist of 25
members, including the Chair,
appointed by the Director, NCI.
Members shall be authorities
knowledgeable in the fields of
community, surgical, medical, and
radiation oncology, patient advocacy,
extramural clinical investigation,
regulatory agencies, pharmaceutical
industry, public health, clinical trials
design, management and evaluation,
drug development and developmental
therapeutics, cancer prevention and
VerDate Aug<31>2005
15:32 Mar 29, 2006
Jkt 208001
control research in the fields of interest
to NCI.
Duration of this committee is
continuing unless formally determined
by the Director, NCI that termination
would be in the best public interest.
Dated: March 21, 2006.
Elias A. Zerhouni,
Director, National Institutes of Health.
[FR Doc. 06–3096 Filed 3–29–06; 8:45 am]
BILLING CODE 4140–01–M
DEPARTMENT OF HEALTH AND
HUMAN SERVICES
National Institutes of Health
Government-Owned Inventions;
Availability for Licensing
National Institutes of Health,
Public Health Service, HHS.
ACTION: Notice.
AGENCY:
SUMMARY: The inventions listed below
are owned by an agency of the U.S.
Government and are available for
licensing in the U.S. in accordance with
35 U.S.C. 207 to achieve expeditious
commercialization of results of
federally-funded research and
development. Foreign patent
applications are filed on selected
inventions to extend market coverage
for companies and may also be available
for licensing.
ADDRESSES: Licensing information and
copies of the U.S. patent applications
listed below may be obtained by writing
to the indicated licensing contact at the
Office of Technology Transfer, National
Institutes of Health, 6011 Executive
Boulevard, Suite 325, Rockville,
Maryland 20852–3804; telephone: 301/
496–7057; fax: 301/402–0220. A signed
Confidential Disclosure Agreement will
be required to receive copies of the
patent applications.
Immunogenic Peptides and Methods of
Use for Treating and Preventing Cancer
Jay A. Berzofsky et al. (NCI)
U.S. Provisional Application No. 60/
773,319 filed 03 Nov 2005 (HHS
Reference No. E–312–2005/0–US–01)
Licensing Contact: John Stansberry; 301/
435–5236; stansbej@mail.nih.gov.
Rhabdomyosarcoma is a malignant
(cancerous), soft tissue tumor found in
children. The most common sites are
the structures of the head and neck, the
urogenital tract, and the arms or legs.
The inventors have discovered an
epitope that is created by a
chromosomal translocation that occurs
in about 80% of alveolar
rhabdomyosarcoma and can elicit a
human cytotoxic T lymphocytes (CTL)
PO 00000
Frm 00057
Fmt 4703
Sfmt 4703
16169
response in individuals who express
HLA–B7.
Many tumors express mutated tumor
associated antigens that often contain Tlymphocyte epitopes. However, the
immune system often remains incapable
of overtaking the growth potential of the
malignant cells. Previous attempts to
obtain protective and therapeutic antitumor immunity have been moderately
successful (Dagher et al., Med Pediatr
Oncol 38: 158–164 (2002) and Rodeberg
et al., Cancer Immuno Immunother 54:
526–534 (2005)). This present invention
seeks to improve on previous attempts
by providing more immunogenic
peptides that bind to a Major
Histocompatibility Complex (MHC)
Class I molecule with higher affinity,
and fusion proteins comprising at least
one of the inventive immunogenic
peptides. This discovery involves
human T-cell responses to human
tumors.
The National Cancer Institute
welcomes statements of capability or
interest from parties interested in
collaborative research to further
develop, evaluate, or commercialize
NCI’s technology related to methods of
protective and therapeutic
immunogenic peptides. Please contact
Dr. Patrick Twomey at 301–496–0477 or
twomeyp@mail.nih.gov for more
information.
Impaired Neuregulin1-Stimulated B
Lymphoblast Migration as Diagnostic
for Schizophrenia
Daniel Weinberger et al. (NIMH)
U.S. Provisional Application No. 60/
735,353 filed 10 Nov 2005 (HHS
Reference No. E–181–2005/1–US–01)
Licensing Contact: Norbert Pontzer; 301/
435–5502; pontzern@mail.nih.gov.
Schizophrenia may be a
neurodevelopmental disorder
(Weinberger D.R. and Marenco S. in
Schizophrenia as a neurodevelopmental
disorder, Hirsch S., Weinberger D.R.
(eds) Schizophrenia, 2nd ed., Blackwell
Science: Oxford, UK, 2003 pp 326–348).
Neuregulin1 (NRG1) plays a critical role
in neuronal migration and maturation
by interacting with ErbB tyrosine kinase
receptors and linkage studies and
genetically engineered animals have
implicated NRG1-mediated signaling in
the neuropathogenesis of schizophrenia.
Although no technique is available to
assess NRG1/ErbB mediated neural
migration in living human brain, there
is increasing recognition that neuronal
cells and immune cells share many
cellular and molecular mechanisms for
cell migration and motility. These
inventors showed NRG1 mediated
chemotactic responses of B lymphocytes
from schizophrenic patients are
E:\FR\FM\30MRN1.SGM
30MRN1
16170
Federal Register / Vol. 71, No. 61 / Thursday, March 30, 2006 / Notices
cprice-sewell on PROD1PC66 with NOTICES
significantly decreased compared to
controls. If aberrant ErbB function
during development is a cause of
schizophrenia, and that aberrant ErbB
function is expressed in peripheral
blood cells throughout life, the assay
should predict susceptibility to
schizophrenia even before clinical
symptoms are apparent.
The NIMH Clinical Brain Disorders
Branch is seeking statements of
capability or interest from parties
interested in collaborative research to
further develop, evaluate, or
commercialize the above technology.
Please contact Suzanne L. Winfield at
winfieldS@mail.nih.gov for more
information.
Treatment of Pulmonary Hypertension
(PH) Using Nitrite Therapy
M. Gladwin (CC), R. Cannon (NHLBI),
A. Schechter (NIDDK), C. Hunter (CC),
R. Pluta (NINDS), E. Oldfield (NINDS)
et al.
PCT Applications filed 09 Jul 2004
(priority date 9 July 2003): PCT/US04/
21985, International Publication No.
WO 2005/007173, Publication Date 27
January 2005 [HHS Reference No. E–
254–2003/2–PCT–01] and PCT/US04/
22232, International Publication No.
WO 2005/004884, Publication Date 20
January 2005 [HHS E–254–2003/3–
PCT–01]
Licensing Contact: Susan Carson,
D.Phil.; 301/435–5020;
carsonsu@mail.nih.gov.
Pulmonary Hypertension (PH) occurs
as a primary or idiopathic disease as
well as secondary to a number of
pulmonary and systemic diseases, such
as neonatal PH and sickle cell disease.
There is no cure for pulmonary
hypertension, a nitric-oxide deficient
state characterized by pulmonary
vasoconstriction and systemic
hypoxemia and therapies vary in
efficacy and cost. Recent studies by NIH
researchers and their collaborators
provided evidence that the blood anion
nitrite contributes to hypoxic
vasodilation through a heme-based,
nitric oxide (NO)-generating reaction
with deoxyhemoglobin and potentially
other heme proteins [Nature Medicine
2003 9:1498–1505]. These initial results
indicate that sodium nitrite can be used
as a potential cost-effective platform
therapy for a wide variety of disease
indications characterized broadly by
constricted blood flow or hypoxia.
These results have been further
corroborated by more recent work in the
neonatal lamb model for PH. Inhaled
sodium nitrite delivered by aerosol to
newborn lambs with hypoxic
pulmonary hypertension elicited a rapid
and sustained reduction (65%) in
VerDate Aug<31>2005
18:18 Mar 29, 2006
Jkt 208001
hypoxia-induced pulmonary
hypertension. Pulmonary vasodilation
elicited by aerosolized nitrite was
deoxyhemoglobin- and pH-dependent
and was associated with increased
blood levels of iron-nitrosylhemoglobin. Notably, short term
delivery of nitrite dissolved in saline
through nebulization produced
selective, sustained pulmonary
vasodilation with no clinically
significant increase in blood
methemoglobin levels. [Nature
Medicine 2004 10:1122–1127]. This
new, simple and cost-effective potential
therapy for neonatal PH is available for
licensing.
Also available for licensing are claims
directed to nitrite salt formulations
associated with elevated blood pressure,
decreased blood flow or hemolytic
disease (HHS Ref. No. E–254–2003/2) as
well as for the treatment of specific
conditions including hepatic, cardiac or
brain ischemia-reperfusion injury and
other cardiovascular conditions [J. Clin.
Invest. (2005) 115:1232–1240; JAMA
(2005) 293:1477–1484] (HHS Ref. No. E–
254–2003/3).
The National Heart, Lung, and Blood
Institute, Vascular Medicine Branch, is
seeking statements of capability or
interest from parties interested in
collaborative research to further
develop, evaluate, or commercialize a
treatment of pulmonary hypertension
(PH) using nitrite therapy. Please
contact Dr. Mark Gladwin by phone at
301–435–2310 or by e-mail at
mgladwin@nih.gov for more
information.
Modified Growth Hormone
YP Loh, NX Cawley (both of NICHD), BJ
Baum (NIDCR), and CR Snell
U.S. Patent Application No. 10/477,651
filed 14 Nov 2003 (HHS Reference No.
E–184–2001/1–US–02) which is a 371
application of PCT/US02/15172 filed
14 May 2002 and which claims
priority to 60/290,836 filed 14 May
2001
Licensing Contact: Susan S. Rucker;
301/435–4478;
ruckersu@mail.nih.gov.
This invention described and claimed
in this patent application provides for
an improved method for producing
human growth hormone (hGH) in vitro
or in vivo. In particular, the patent
application describes compositions and
methods which are based on a modified
form of human growth hormone where
the regulated secretory pathway (RSP)
sorting signal has been modified to
provide for the constitutive secretion of
human growth hormone via the
nonregulated secretory pathway (NRSP)
in a mammalian cell. One particular
PO 00000
Frm 00058
Fmt 4703
Sfmt 4703
modified hGH composition, has been
demonstrated to be biologically active
and able to be secreted into the
bloodstream in an animal model
providing proof-of-concept. This
invention can be applied to a noninvasive method of gene therapy to
achieve sustained delivery of this
therapeutic protein.
The application has been published as
WO 02/092619 (11/21/2002) and as
2004/0158046 A1 (08/12/2004). The
work has also been published at Wang
J, et al. Human Gene Therapy 16(5):571–
83 (May 2005). Only U.S. Patent
protection has been sought for this
technology. There are no foreign
counterpart patent applications.
The NICHD Office of the Scientific
Director is seeking statements of
capability or interest from parties
interested in collaborative research to
further develop, evaluate, or
commercialize the non-invasive method
of production and systemic delivery of
growth hormone or other proteins for
therapeutic purposes. Please contact Dr.
Y. Peng Loh at 301/496–3239 or
lohp@mail.nih.gov for more
information.
Dated: March 21, 2006.
Steven M. Ferguson,
Director, Division of Technology Development
and Transfer, Office of Technology Transfer,
National Institutes of Health.
[FR Doc. E6–4611 Filed 3–29–06; 8:45 am]
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DEPARTMENT OF HEALTH AND
HUMAN SERVICES
National Institutes of Health
Office of the Director, National
Institutes of Health, Notice of Meeting
Pursuant to section 10(a) of the
Federal Advisory Committee Act, as
amended (5 U.S.C. Appendix 2), notice
is hereby given of a meeting of the
Director’s Council of Public
Representatives.
The meeting will be open to the
public, with attendance limited to space
available. Individuals who plan to
attend and need special assistance, such
as sign language interpretation or other
reasonable accommodations, should
notify the Contact Person listed below
in advance of the meeting.
Name of Committee: Director’s Council of
Public Representatives.
Date: April 21, 2006.
Time: 8:30 a.m. to 5 p.m.
Agenda: Among the topics proposed for
discussion are: (1) NIH Director’s Update; (2)
the NIH Peer Review Process and
Opportunities for Public Participation; (3)
NIH Clinical Research Education and
E:\FR\FM\30MRN1.SGM
30MRN1
]]>Agencies
[Federal Register Volume 71, Number 61 (Thursday, March 30, 2006)]
[Notices]
[Pages 16169-16170]
From the Federal Register Online via the Government Printing Office [www.gpo.gov]
[FR Doc No: E6-4611]
-----------------------------------------------------------------------
DEPARTMENT OF HEALTH AND HUMAN SERVICES
National Institutes of Health
Government-Owned Inventions; Availability for Licensing
AGENCY: National Institutes of Health, Public Health Service, HHS.
ACTION: Notice.
-----------------------------------------------------------------------
SUMMARY: The inventions listed below are owned by an agency of the U.S.
Government and are available for licensing in the U.S. in accordance
with 35 U.S.C. 207 to achieve expeditious commercialization of results
of federally-funded research and development. Foreign patent
applications are filed on selected inventions to extend market coverage
for companies and may also be available for licensing.
ADDRESSES: Licensing information and copies of the U.S. patent
applications listed below may be obtained by writing to the indicated
licensing contact at the Office of Technology Transfer, National
Institutes of Health, 6011 Executive Boulevard, Suite 325, Rockville,
Maryland 20852-3804; telephone: 301/496-7057; fax: 301/402-0220. A
signed Confidential Disclosure Agreement will be required to receive
copies of the patent applications.
Immunogenic Peptides and Methods of Use for Treating and Preventing
Cancer
Jay A. Berzofsky et al. (NCI)
U.S. Provisional Application No. 60/773,319 filed 03 Nov 2005 (HHS
Reference No. E-312-2005/0-US-01)
Licensing Contact: John Stansberry; 301/435-5236;
stansbej@mail.nih.gov.
Rhabdomyosarcoma is a malignant (cancerous), soft tissue tumor
found in children. The most common sites are the structures of the head
and neck, the urogenital tract, and the arms or legs. The inventors
have discovered an epitope that is created by a chromosomal
translocation that occurs in about 80% of alveolar rhabdomyosarcoma and
can elicit a human cytotoxic T lymphocytes (CTL) response in
individuals who express HLA-B7.
Many tumors express mutated tumor associated antigens that often
contain T-lymphocyte epitopes. However, the immune system often remains
incapable of overtaking the growth potential of the malignant cells.
Previous attempts to obtain protective and therapeutic anti-tumor
immunity have been moderately successful (Dagher et al., Med Pediatr
Oncol 38: 158-164 (2002) and Rodeberg et al., Cancer Immuno Immunother
54: 526-534 (2005)). This present invention seeks to improve on
previous attempts by providing more immunogenic peptides that bind to a
Major Histocompatibility Complex (MHC) Class I molecule with higher
affinity, and fusion proteins comprising at least one of the inventive
immunogenic peptides. This discovery involves human T-cell responses to
human tumors.
The National Cancer Institute welcomes statements of capability or
interest from parties interested in collaborative research to further
develop, evaluate, or commercialize NCI's technology related to methods
of protective and therapeutic immunogenic peptides. Please contact Dr.
Patrick Twomey at 301-496-0477 or twomeyp@mail.nih.gov for more
information.
Impaired Neuregulin1-Stimulated B Lymphoblast Migration as Diagnostic
for Schizophrenia
Daniel Weinberger et al. (NIMH)
U.S. Provisional Application No. 60/735,353 filed 10 Nov 2005 (HHS
Reference No. E-181-2005/1-US-01)
Licensing Contact: Norbert Pontzer; 301/435-5502;
pontzern@mail.nih.gov.
Schizophrenia may be a neurodevelopmental disorder (Weinberger D.R.
and Marenco S. in Schizophrenia as a neurodevelopmental disorder,
Hirsch S., Weinberger D.R. (eds) Schizophrenia, 2nd ed., Blackwell
Science: Oxford, UK, 2003 pp 326-348). Neuregulin1 (NRG1) plays a
critical role in neuronal migration and maturation by interacting with
ErbB tyrosine kinase receptors and linkage studies and genetically
engineered animals have implicated NRG1-mediated signaling in the
neuropathogenesis of schizophrenia. Although no technique is available
to assess NRG1/ErbB mediated neural migration in living human brain,
there is increasing recognition that neuronal cells and immune cells
share many cellular and molecular mechanisms for cell migration and
motility. These inventors showed NRG1 mediated chemotactic responses of
B lymphocytes from schizophrenic patients are
[[Page 16170]]
significantly decreased compared to controls. If aberrant ErbB function
during development is a cause of schizophrenia, and that aberrant ErbB
function is expressed in peripheral blood cells throughout life, the
assay should predict susceptibility to schizophrenia even before
clinical symptoms are apparent.
The NIMH Clinical Brain Disorders Branch is seeking statements of
capability or interest from parties interested in collaborative
research to further develop, evaluate, or commercialize the above
technology. Please contact Suzanne L. Winfield at
winfieldS@mail.nih.gov for more information.
Treatment of Pulmonary Hypertension (PH) Using Nitrite Therapy
M. Gladwin (CC), R. Cannon (NHLBI), A. Schechter (NIDDK), C. Hunter
(CC), R. Pluta (NINDS), E. Oldfield (NINDS) et al.
PCT Applications filed 09 Jul 2004 (priority date 9 July 2003): PCT/
US04/21985, International Publication No. WO 2005/007173, Publication
Date 27 January 2005 [HHS Reference No. E-254-2003/2-PCT-01] and PCT/
US04/22232, International Publication No. WO 2005/004884, Publication
Date 20 January 2005 [HHS E-254-2003/3-PCT-01]
Licensing Contact: Susan Carson, D.Phil.; 301/435-5020;
carsonsu@mail.nih.gov.
Pulmonary Hypertension (PH) occurs as a primary or idiopathic
disease as well as secondary to a number of pulmonary and systemic
diseases, such as neonatal PH and sickle cell disease. There is no cure
for pulmonary hypertension, a nitric-oxide deficient state
characterized by pulmonary vasoconstriction and systemic hypoxemia and
therapies vary in efficacy and cost. Recent studies by NIH researchers
and their collaborators provided evidence that the blood anion nitrite
contributes to hypoxic vasodilation through a heme-based, nitric oxide
(NO)-generating reaction with deoxyhemoglobin and potentially other
heme proteins [Nature Medicine 2003 9:1498-1505]. These initial results
indicate that sodium nitrite can be used as a potential cost-effective
platform therapy for a wide variety of disease indications
characterized broadly by constricted blood flow or hypoxia.
These results have been further corroborated by more recent work in
the neonatal lamb model for PH. Inhaled sodium nitrite delivered by
aerosol to newborn lambs with hypoxic pulmonary hypertension elicited a
rapid and sustained reduction (65%) in hypoxia-induced pulmonary
hypertension. Pulmonary vasodilation elicited by aerosolized nitrite
was deoxyhemoglobin- and pH-dependent and was associated with increased
blood levels of iron-nitrosyl-hemoglobin. Notably, short term delivery
of nitrite dissolved in saline through nebulization produced selective,
sustained pulmonary vasodilation with no clinically significant
increase in blood methemoglobin levels. [Nature Medicine 2004 10:1122-
1127]. This new, simple and cost-effective potential therapy for
neonatal PH is available for licensing.
Also available for licensing are claims directed to nitrite salt
formulations associated with elevated blood pressure, decreased blood
flow or hemolytic disease (HHS Ref. No. E-254-2003/2) as well as for
the treatment of specific conditions including hepatic, cardiac or
brain ischemia-reperfusion injury and other cardiovascular conditions
[J. Clin. Invest. (2005) 115:1232-1240; JAMA (2005) 293:1477-1484] (HHS
Ref. No. E-254-2003/3).
The National Heart, Lung, and Blood Institute, Vascular Medicine
Branch, is seeking statements of capability or interest from parties
interested in collaborative research to further develop, evaluate, or
commercialize a treatment of pulmonary hypertension (PH) using nitrite
therapy. Please contact Dr. Mark Gladwin by phone at 301-435-2310 or by
e-mail at mgladwin@nih.gov for more information.
Modified Growth Hormone
YP Loh, NX Cawley (both of NICHD), BJ Baum (NIDCR), and CR Snell
U.S. Patent Application No. 10/477,651 filed 14 Nov 2003 (HHS Reference
No. E-184-2001/1-US-02) which is a 371 application of PCT/US02/15172
filed 14 May 2002 and which claims priority to 60/290,836 filed 14 May
2001
Licensing Contact: Susan S. Rucker; 301/435-4478;
ruckersu@mail.nih.gov.
This invention described and claimed in this patent application
provides for an improved method for producing human growth hormone
(hGH) in vitro or in vivo. In particular, the patent application
describes compositions and methods which are based on a modified form
of human growth hormone where the regulated secretory pathway (RSP)
sorting signal has been modified to provide for the constitutive
secretion of human growth hormone via the nonregulated secretory
pathway (NRSP) in a mammalian cell. One particular modified hGH
composition, has been demonstrated to be biologically active and able
to be secreted into the bloodstream in an animal model providing proof-
of-concept. This invention can be applied to a non-invasive method of
gene therapy to achieve sustained delivery of this therapeutic protein.
The application has been published as WO 02/092619 (11/21/2002) and
as 2004/0158046 A1 (08/12/2004). The work has also been published at
Wang J, et al. Human Gene Therapy 16(5):571-83 (May 2005). Only U.S.
Patent protection has been sought for this technology. There are no
foreign counterpart patent applications.
The NICHD Office of the Scientific Director is seeking statements
of capability or interest from parties interested in collaborative
research to further develop, evaluate, or commercialize the non-
invasive method of production and systemic delivery of growth hormone
or other proteins for therapeutic purposes. Please contact Dr. Y. Peng
Loh at 301/496-3239 or lohp@mail.nih.gov for more information.
Dated: March 21, 2006.
Steven M. Ferguson,
Director, Division of Technology Development and Transfer, Office of
Technology Transfer, National Institutes of Health.
[FR Doc. E6-4611 Filed 3-29-06; 8:45 am]
BILLING CODE 4140-01-P
