Government-Owned Invention; Availability for Licensing, 22553 [2017-09791]
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Federal Register / Vol. 82, No. 93 / Tuesday, May 16, 2017 / Notices
Health, 6701 Rockledge Drive, Room 6194,
MSC 7804, Bethesda, MD 20892, 301–594–
7945, smileyja@csr.nih.gov.
Name of Committee: Musculoskeletal, Oral
and Skin Sciences Integrated Review Group;
Arthritis, Connective Tissue and Skin Study
Section.
Date: June 12–13, 2017.
Time: 8:00 a.m. to 5:00 p.m.
Agenda: To review and evaluate grant
applications.
Place: Hilton Long Beach and Executive
Center, 701 West Ocean Boulevard, Long
Beach, CA 90831.
Contact Person: Alexey Belkin, Ph.D.,
Scientific Review Officer, Center for
Scientific Review, National Institutes of
Health, 6701 Rockledge Drive, Room 4102,
Bethesda, MD 20817, 301–435–1786,
alexey.belkin@nih.gov.
Name of Committee: Infectious Diseases
and Microbiology Integrated Review Group;
Clinical Research and Field Studies of
Infectious Diseases Study Section.
Date: June 12–13, 2017.
Time: 8:30 a.m. to 5:00 p.m.
Agenda: To review and evaluate grant
applications.
Place: Cambria Hotel and Suites, 1 Helen
Heneghan Way, Rockville, MD 20850.
Contact Person: Soheyla Saadi, Ph.D.,
Scientific Review Officer, Center for
Scientific Review, National Institutes of
Health, 6701 Rockledge Drive, Room 3211,
MSC 7808, Bethesda, MD 20892, 301–435–
0903, saadisoh@csr.nih.gov.
(Catalogue of Federal Domestic Assistance
Program Nos. 93.306, Comparative Medicine;
93.333, Clinical Research, 93.306, 93.333,
93.337, 93.393–93.396, 93.837–93.844,
93.846–93.878, 93.892, 93.893, National
Institutes of Health, HHS)
Dated: May 10, 2017.
David Clary,
Program Analyst, Office of Federal Advisory
Committee Policy.
[FR Doc. 2017–09780 Filed 5–15–17; 8:45 am]
BILLING CODE 4140–01–P
DEPARTMENT OF HEALTH AND
HUMAN SERVICES
National Institutes of Health
Government-Owned Invention;
Availability for Licensing
AGENCY:
National Institutes of Health,
HHS.
ACTION:
Notice.
The inventions listed below
are owned by an agency of the U.S.
Government.
sradovich on DSK3GMQ082PROD with NOTICES
SUMMARY:
FOR FURTHER INFORMATION CONTACT:
Licensing information may be obtained
by emailing the indicated licensing
contact at the National Heart, Lung, and
Blood, Office of Technology Transfer
and Development Office of Technology
Transfer, 31 Center Drive Room 4A29,
VerDate Sep<11>2014
16:42 May 15, 2017
Jkt 241001
MSC 2479, Bethesda, MD 20892–2479;
telephone: 301–402–5579. A signed
Confidential Disclosure Agreement may
be required to receive any unpublished
information.
SUPPLEMENTARY INFORMATION: The
following inventions are available for
licensing in accordance with 35 U.S.C.
209 and 37 CFR part 404 to achieve
expeditious commercialization of
results of federally-funded research and
development. Technology description
follows.
Efficient mRNA-Based Genetic
Engineering of Human NK Cells With
High-Affinity CD16 and CCR7
Description of Technology: A highly
efficient method to genetically modify
natural killer (NK) cells to induce
expression of high affinity CD16 (HA–
CD16) through mRNA electroporation,
to potentiate NK cell-mediated
antibody-dependent cellular
cytotoxicity (ADCC). ADCC is mediated
by CD16+ NK cells following adoptive
NK cell transfer, but most humans
express CD16 which has a relatively low
affinity for IgG1 antibodies. However, a
single nucleotide polymorphism (SNP
rs396991) in the CD16 gene, resulting in
an amino acid substitution at position
158 (F158V), is associated with
substantially higher affinity and
superior NK cell-mediated ADCC than
those with the 158F genotype. This HA–
CD16–158V polymorphism has also
been linked to enhanced ADCC capacity
in vivo. The nearly 100% efficiency of
our method resulted in: (a) Sustained
surface expression of transgenes at high
levels for up to 4 days without
compromising NK cell cytotoxicity and
viability; and (b) augmented ADCC
against Daratumumab coated multiple
myeloma cells by ex vivo expanded NK
cells electroporated with mRNA coding
for HA–CD16. This system is GMP
compliant and has been used previously
in FDA approved clinical trials.
Potential Commercial Applications:
Infusion of a large number of highly
cytotoxic autologous ex vivo expanded
NK cells expressing high-affinity CD16
into patients, to induce a more profound
anti-malignancy response to specific
monoclonal antibodies, including:
multiple myeloma (Daratumumab);
lymphoma (Rituximab); breast cancer
(Trastuzumab); and colon cancer
(Cetuximab).
Development Stage: Early-stage; In
vitro data available.
Inventors: Richard W. Childs and
Mattias Carlsten (NHLBI).
Publications:
(1) Carlsten M, Levy E, Karambelkar
A, Li L, Reger R, Berg M, Peshwa MV
and Childs RW (2016) Efficient mRNA-
PO 00000
Frm 00077
Fmt 4703
Sfmt 4703
22553
Based Genetic Engineering of Human
NK Cells with High-Affinity CD16 and
CCR7 Augments Rituximab-Induced
ADCC against Lymphoma and Targets
NK Cell Migration toward the Lymph
Node-Associated Chemokine CCL19.
Front. Immunol. 7:105. doi: 10.3389/
fimmu.2016.00105.
(2) Carlsten M and Childs RW (2015)
Genetic manipulation of NK cells for
cancer immunotherapy: techniques and
clinical implications. Front. Immunol.
6:266. doi: 10.3389/fimmu.2015.00266.
Intellectual Property: NIH Reference
No. E–036–2015/0,1—US Application
No. 62/079,975, filed 14 Nov 2014; and
PCT Application No. PCT/US2015/
060646, filed 13 Nov 2015.
Licensing Contact: Cristina
Thalhammer-Reyero, Ph.D., M.B.A.;
301–435–4507; thalhamc@mail.nih.gov.
Dated: May 4, 2017.
Cristina Thalhammer-Reyero,
Senior Licensing and Patenting Manager,
Office of Technology Transfer and
Development, National Heart, Lung, and
Blood Institute.
[FR Doc. 2017–09791 Filed 5–15–17; 8:45 am]
BILLING CODE 4140–01–P
DEPARTMENT OF HEALTH AND
HUMAN SERVICES
National Institutes of Health
National Institute on Minority Health
and Health Disparities; Notice of
Closed Meeting
Pursuant to section 10(d) of the
Federal Advisory Committee Act, as
amended (5 U.S.C. App.), notice is
hereby given of the following meeting.
The meeting will be closed to the
public in accordance with the
provisions set forth in sections
552b(c)(4) and 552b(c)(6), Title 5 U.S.C.,
as amended. The grant applications and
the discussions could disclose
confidential trade secrets or commercial
property such as patentable materials,
and personal information concerning
individuals associated with the grant
applications, the disclosure of which
would constitute a clearly unwarranted
invasion of personal privacy.
Name of Committee: National Institute on
Minority Health and Health Disparities,
Special Emphasis Panel; NIH Support for
Conferences and Scientific Meeting—DRI
(01).
Date: June 19, 2017.
Time: 8:00 a.m. to 5:00 p.m.
Agenda: To review and evaluate grant
applications.
Place: National Institutes of Health,
Gateway Plaza, 533J, 7201 Wisconsin
Avenue, Suite 533, Bethesda, MD 20814
(Teleconference).
E:\FR\FM\16MYN1.SGM
16MYN1
]]>Agencies
[Federal Register Volume 82, Number 93 (Tuesday, May 16, 2017)]
[Notices]
[Page 22553]
From the Federal Register Online via the Government Publishing Office [www.gpo.gov]
[FR Doc No: 2017-09791]
-----------------------------------------------------------------------
DEPARTMENT OF HEALTH AND HUMAN SERVICES
National Institutes of Health
Government-Owned Invention; Availability for Licensing
AGENCY: National Institutes of Health, HHS.
ACTION: Notice.
-----------------------------------------------------------------------
SUMMARY: The inventions listed below are owned by an agency of the U.S.
Government.
FOR FURTHER INFORMATION CONTACT: Licensing information may be obtained
by emailing the indicated licensing contact at the National Heart,
Lung, and Blood, Office of Technology Transfer and Development Office
of Technology Transfer, 31 Center Drive Room 4A29, MSC 2479, Bethesda,
MD 20892-2479; telephone: 301-402-5579. A signed Confidential
Disclosure Agreement may be required to receive any unpublished
information.
SUPPLEMENTARY INFORMATION: The following inventions are available for
licensing in accordance with 35 U.S.C. 209 and 37 CFR part 404 to
achieve expeditious commercialization of results of federally-funded
research and development. Technology description follows.
Efficient mRNA-Based Genetic Engineering of Human NK Cells With High-
Affinity CD16 and CCR7
Description of Technology: A highly efficient method to genetically
modify natural killer (NK) cells to induce expression of high affinity
CD16 (HA-CD16) through mRNA electroporation, to potentiate NK cell-
mediated antibody-dependent cellular cytotoxicity (ADCC). ADCC is
mediated by CD16\+\ NK cells following adoptive NK cell transfer, but
most humans express CD16 which has a relatively low affinity for IgG1
antibodies. However, a single nucleotide polymorphism (SNP rs396991) in
the CD16 gene, resulting in an amino acid substitution at position 158
(F158V), is associated with substantially higher affinity and superior
NK cell-mediated ADCC than those with the 158F genotype. This HA-CD16-
158V polymorphism has also been linked to enhanced ADCC capacity in
vivo. The nearly 100% efficiency of our method resulted in: (a)
Sustained surface expression of transgenes at high levels for up to 4
days without compromising NK cell cytotoxicity and viability; and (b)
augmented ADCC against Daratumumab coated multiple myeloma cells by ex
vivo expanded NK cells electroporated with mRNA coding for HA-CD16.
This system is GMP compliant and has been used previously in FDA
approved clinical trials.
Potential Commercial Applications: Infusion of a large number of
highly cytotoxic autologous ex vivo expanded NK cells expressing high-
affinity CD16 into patients, to induce a more profound anti-malignancy
response to specific monoclonal antibodies, including: multiple myeloma
(Daratumumab); lymphoma (Rituximab); breast cancer (Trastuzumab); and
colon cancer (Cetuximab).
Development Stage: Early-stage; In vitro data available.
Inventors: Richard W. Childs and Mattias Carlsten (NHLBI).
Publications:
(1) Carlsten M, Levy E, Karambelkar A, Li L, Reger R, Berg M,
Peshwa MV and Childs RW (2016) Efficient mRNA-Based Genetic Engineering
of Human NK Cells with High-Affinity CD16 and CCR7 Augments Rituximab-
Induced ADCC against Lymphoma and Targets NK Cell Migration toward the
Lymph Node-Associated Chemokine CCL19. Front. Immunol. 7:105. doi:
10.3389/fimmu.2016.00105.
(2) Carlsten M and Childs RW (2015) Genetic manipulation of NK
cells for cancer immunotherapy: techniques and clinical implications.
Front. Immunol. 6:266. doi: 10.3389/fimmu.2015.00266.
Intellectual Property: NIH Reference No. E-036-2015/0,1--US
Application No. 62/079,975, filed 14 Nov 2014; and PCT Application No.
PCT/US2015/060646, filed 13 Nov 2015.
Licensing Contact: Cristina Thalhammer-Reyero, Ph.D., M.B.A.; 301-
435-4507; thalhamc@mail.nih.gov.
Dated: May 4, 2017.
Cristina Thalhammer-Reyero,
Senior Licensing and Patenting Manager, Office of Technology Transfer
and Development, National Heart, Lung, and Blood Institute.
[FR Doc. 2017-09791 Filed 5-15-17; 8:45 am]
BILLING CODE 4140-01-P
