Determination of Regulatory Review Period for Purposes of Patent Extension; ATRYN, 15323-15324 [2011-6509]
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Federal Register / Vol. 76, No. 54 / Monday, March 21, 2011 / Notices
Interested persons may submit to the
Division of Dockets Management (see
ADDRESSES) electronic or written
comments and written petitions. It is
only necessary to send one set of
comments. It is no longer necessary to
send three copies of mailed comments.
However, if you submit a written
petition, you must submit three copies
of the petition. Identify comments with
the docket number found in brackets in
the heading of this document.
Comments and petitions that have not
been made publicly available on
https://www.regulations.gov may be
viewed in the Division of Dockets
Management between 9 a.m. and 4 p.m.,
Monday through Friday.
Dated: February 14, 2011.
Jane A. Axelrad,
Associate Director for Policy, Center for Drug
Evaluation and Research.
[FR Doc. 2011–6514 Filed 3–18–11; 8:45 am]
BILLING CODE 4160–01–P
DEPARTMENT OF HEALTH AND
HUMAN SERVICES
Food and Drug Administration
[Docket No. FDA–2010–E–0241]
Determination of Regulatory Review
Period for Purposes of Patent
Extension; ATRYN
AGENCY:
Food and Drug Administration,
HHS.
ACTION:
Notice.
The Food and Drug
Administration (FDA) has determined
the regulatory review period for ATRYN
and is publishing this notice of that
determination as required by law. FDA
has made the determination because of
the submission of an application to the
Director of Patents and Trademarks,
Department of Commerce, for the
extension of a patent which claims that
human biological product.
ADDRESSES: Submit electronic
comments to https://
www.regulations.gov. Submit written
petitions along with three copies and
written comments to the Division of
Dockets Management (HFA–305), Food
and Drug Administration, 5630 Fishers
Lane, rm. 1061, Rockville, MD 20852.
FOR FURTHER INFORMATION CONTACT:
Beverly Friedman, Office of Regulatory
Policy, Food and Drug Administration,
10903 New Hampshire Ave., Bldg. 51,
rm. 6222, Silver Spring, MD 20993–
0002. 301–796–3602.
SUPPLEMENTARY INFORMATION: The Drug
Price Competition and Patent Term
Restoration Act of 1984 (Pub. L. 98–417)
mstockstill on DSKH9S0YB1PROD with NOTICES
SUMMARY:
VerDate Mar<15>2010
17:50 Mar 18, 2011
Jkt 223001
and the Generic Animal Drug and Patent
Term Restoration Act (Pub. L. 100–670)
generally provide that a patent may be
extended for a period of up to 5 years
so long as the patented item (human
drug product, animal drug product,
medical device, food additive, or color
additive) was subject to regulatory
review by FDA before the item was
marketed. Under these acts, a product’s
regulatory review period forms the basis
for determining the amount of extension
an applicant may receive.
A regulatory review period consists of
two periods of time: A testing phase and
an approval phase. For human
biological products, the testing phase
begins when the exemption to permit
the clinical investigations of the
biological becomes effective and runs
until the approval phase begins. The
approval phase starts with the initial
submission of an application to market
the human biological product and
continues until FDA grants permission
to market the biological product.
Although only a portion of a regulatory
review period may count toward the
actual amount of extension that the
Director of Patents and Trademarks may
award (for example, half the testing
phase must be subtracted as well as any
time that may have occurred before the
patent was issued), FDA’s determination
of the length of a regulatory review
period for a human biological product
will include all of the testing phase and
approval phase as specified in 35 U.S.C.
156(g)(1)(B).
FDA recently approved for marketing
the human biologic product ATRYN
(antithrombin (recombinant)). ATRYN is
indicated for the prevention of perioperative and peri-partum
thromboembolic events in hereditary
antithrombin deficient patients.
Subsequent to this approval, the Patent
and Trademark Office received a patent
term restoration application for ATRYN
(U.S. Patent No. 6,441,145) from GTC
Biotherapeutics, Inc., and the Patent and
Trademark Office requested FDA’s
assistance in determining this patent’s
eligibility for patent term restoration. In
a letter dated February 17, 2010, FDA
advised the Patent and Trademark
Office that this human biological
product had undergone a regulatory
review period and that the approval of
ATRYN represented the first permitted
commercial marketing or use of the
recombinant product. Thereafter, the
Patent and Trademark Office requested
that FDA determine the product’s
regulatory review period.
FDA has determined that the
applicable regulatory review period for
ATRYN is 4,468 days. Of this time,
4,285 days occurred during the testing
PO 00000
Frm 00046
Fmt 4703
Sfmt 4703
15323
phase of the regulatory review period,
while 183 days occurred during the
approval phase. These periods of time
were derived from the following dates:
1. The date an exemption under
section 505(i) of the Federal Food, Drug,
and Cosmetic Act (21 U.S.C. 355(i))
became effective: November 15, 1996.
The applicant claims November 14,
1996, as the date the investigational new
drug application (IND) became effective.
However, FDA records indicate that the
IND effective date was November 15,
1996, which was 30 days after FDA
receipt of the IND.
2. The date the application was
initially submitted with respect to the
human biological product under section
351 of the Public Health Service Act (42
U.S.C. 262): August 8, 2008. The
applicant claims January 31, 2008, as
the date the biologics license
application (BLA) for ATRYN (BLA
125284) was initially submitted.
However, FDA records indicate that
BLA 125284 was submitted on August
8, 2008.
3. The date the application was
approved: February 6, 2009. FDA has
verified the applicant’s claim that BLA
125284 was approved on February 6,
2009.
This determination of the regulatory
review period establishes the maximum
potential length of a patent extension.
However, the U.S. Patent and
Trademark Office applies several
statutory limitations in its calculations
of the actual period for patent extension.
In its application for patent extension,
this applicant seeks 1,243 days of patent
term extension.
Anyone with knowledge that any of
the dates as published are incorrect may
submit to the Division of Dockets
Management (see ADDRESSES) either
electronic or written comments and ask
for a redetermination by May 20, 2011.
Furthermore, any interested person may
petition FDA for a determination
regarding whether the applicant for
extension acted with due diligence
during the regulatory review period by
September 19, 2011. To meet its burden,
the petition must contain sufficient facts
to merit an FDA investigation. (See H.
Rept. 857, part 1, 98th Cong., 2d sess.,
pp. 41–42, 1984.) Petitions should be in
the format specified in 21 CFR 10.30.
Interested persons may submit to the
Division of Dockets Management (see
ADDRESSES) electronic or written
comments and written petitions. It is
only necessary to send one set of
comments. It is no longer necessary to
send three copies of mailed comments.
However, if you submit a written
petition, you must submit three copies
of the petition. Identify comments with
E:\FR\FM\21MRN1.SGM
21MRN1
15324
Federal Register / Vol. 76, No. 54 / Monday, March 21, 2011 / Notices
the docket number found in brackets in
the heading of this document.
Comments and petitions that have not
been made publicly available on
https://www.regulations.gov may be
viewed in the Division of Dockets
Management between 9 a.m. and 4 p.m.,
Monday through Friday.
Dated: February 14, 2011.
Jane A. Axelrad,
Associate Director for Policy, Center for Drug
Evaluation and Research.
[FR Doc. 2011–6509 Filed 3–18–11; 8:45 am]
BILLING CODE P
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:
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.
mstockstill on DSKH9S0YB1PROD with NOTICES
SUMMARY:
UOK 268 Cell Line for Hereditary
Leiomyomatosis and Renal Cell
Carcinoma
Description of Technology: Hereditary
Leiomyomatosis and Renal Cell
Carcinoma (HLRCC) is an extremely
aggressive cancer syndrome with no
effective treatment regimen and
currently no cure. The progress of
identifying HLRCC treatments and cures
has likely been hindered due to the lack
of an HLRCC model for studying the
cancer syndrome and for screening
therapeutic drug candidates.
This technology describes the UOK
268 cell line, a spontaneously
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17:50 Mar 18, 2011
Jkt 223001
immortalized renal tumor cell line that
may be of great interest to industry for
studying HLRCC, drug screening, and
searching for tumor markers related to
diagnosis, prognosis, and drug
resistance. This cell line is only the
second spontaneously immortalized
cancer cell line of its kind in the world
and is unique in that it is a primary
tumor cell model (the other cell line,
UOK 262, is from a metastasis cell
model). The UOK 268 cell line is an
established, clonal, immortalized renal
cancer cell line derived from the longterm culture of aggressive tumor tissues
of HLRCC in a specially designed
culture medium under strict culture
conditions. The UOK 268 exhibits an
array of HLRCC kidney cancer
characteristics that can promote protein
and fatty acid biosynthesis and
modulate HIF activities in a manner
conducive to cancer cell proliferation.
Benefits:
• This is only one of two
immortalized HLRCC cell lines, and is
unique in that it is from a primary
tumor cell model.
• Developing a diagnostic to search
for tumor targets and screen for HLRCC
and related cancers drug candidates will
have significant benefits, including
early detection and treatment.
Applications:
• In vitro and in vivo cell model for
understanding the biology of HLRCC
and related cancers, including growth,
motility, invasion, and metabolite
production.
• High throughput screening to test
for drug candidates that could be used
to treat particular cancers, such as
HLRCC.
• Diagnostic tool for the diagnosis,
prognosis, and drug resistance of tumor
markers.
Advantages:
• Cell line is derived from a HLRCC
patient: This cell line is anticipated to
retain many features of primary HLRCC
samples and novel HLRCC antigens
identified from this cell line are likely
to correlate with antigens expressed on
human HLRCC tumors. Studies
performed using this cell lines may have
a direct correlation to the initiation,
progression, treatment, and prevention
of HLRCC in humans.
• Molecular and genetic features are
well characterized: The inventors have
elucidated many physical
characteristics of the cell lines and their
data reveals previously unrecognized
coordination between mammalian
glucose and iron metabolisms through
AMPK signaling, and a novel
mechanism for modulating HIF
activities in renal cancers.
PO 00000
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Fmt 4703
Sfmt 4703
Inventors: W. Marston Linehan and
Youfeng Yang (NCI)
Publications:
1. Youfeng Yang et al. Distinct Mitotranscriptome Profiling in Fumarate
Hydratase-deficient Novel Primary
Tumor Cell Line UOK268 Leads to
Better Understanding of Early Human
HLRCC-associated Cancer with Multiple
Dysregulated Molecular Events and
Metabolic Shunts. Under submission.
2. Wing-Hang Tong et al.
Hypoactivation of AMPK pathway and
remodeling of iron metabolism in
hereditary leiomyomatosis and renal
cell carcinoma tumorigenesis. Under
resubmission.
Patent Status: HHS Reference No. E–
254–2010/0—Research Tool. Patent
protection is not being pursued for this
technology.
Licensing Status: Available for
licensing.
Licensing Contact: Whitney Hastings;
301–451–7337; hastingw@mail.nih.gov.
Collaborative Research Opportunity:
The Center for Cancer Research,
Urologic Oncology Branch, is seeking
statements of capability or interest from
parties interested in collaborative
research to further develop, evaluate, or
commercialize UOK268 as human
HLRCC primary cell line model to
comparing previously established
UOK262, which was from metastasis
lympho node. UOK 268 is a unique cell
model for studying the underlying
molecular derangements associated with
impaired oxidative phosphorylation in
cancer and for evaluating novel
therapeutic approaches for this HLRCCassociated kidney cancer. Please contact
John Hewes, PhD at 301–435–3121 or
hewesj@mail.nih.gov for more
information.
Agonistic Human Monoclonal
Antibodies Against DR4
Description of Technology: The tumor
necrosis factor (TNF)-related apoptosisinducing ligand (TRAIL) and its
functional receptors, DR4 and DR5, have
been recognized as promising targets for
cancer treatment. Therapeutics targeting
TRAIL and its receptors are not only
effective in killing many types of tumors
but they also synergize with traditional
therapies, and show efficacy against
tumors that are otherwise resistant to
conventional treatments.
The researchers at the NIH have
developed two human monoclonal
antibodies (mAbs) that bind to death
receptor 4 (‘‘DR4’’). One of the mAbs is
agonistic and inhibits the growth of
ST486 cells with IC50 of about 10nM.
The two mAbs were selected from a
human phage-displayed Fab library by
panning against a recombinant DR4
E:\FR\FM\21MRN1.SGM
21MRN1
]]>Agencies
[Federal Register Volume 76, Number 54 (Monday, March 21, 2011)]
[Notices]
[Pages 15323-15324]
From the Federal Register Online via the Government Printing Office [www.gpo.gov]
[FR Doc No: 2011-6509]
-----------------------------------------------------------------------
DEPARTMENT OF HEALTH AND HUMAN SERVICES
Food and Drug Administration
[Docket No. FDA-2010-E-0241]
Determination of Regulatory Review Period for Purposes of Patent
Extension; ATRYN
AGENCY: Food and Drug Administration, HHS.
ACTION: Notice.
-----------------------------------------------------------------------
SUMMARY: The Food and Drug Administration (FDA) has determined the
regulatory review period for ATRYN and is publishing this notice of
that determination as required by law. FDA has made the determination
because of the submission of an application to the Director of Patents
and Trademarks, Department of Commerce, for the extension of a patent
which claims that human biological product.
ADDRESSES: Submit electronic comments to https://www.regulations.gov.
Submit written petitions along with three copies and written comments
to the Division of Dockets Management (HFA-305), Food and Drug
Administration, 5630 Fishers Lane, rm. 1061, Rockville, MD 20852.
FOR FURTHER INFORMATION CONTACT: Beverly Friedman, Office of Regulatory
Policy, Food and Drug Administration, 10903 New Hampshire Ave., Bldg.
51, rm. 6222, Silver Spring, MD 20993-0002. 301-796-3602.
SUPPLEMENTARY INFORMATION: The Drug Price Competition and Patent Term
Restoration Act of 1984 (Pub. L. 98-417) and the Generic Animal Drug
and Patent Term Restoration Act (Pub. L. 100-670) generally provide
that a patent may be extended for a period of up to 5 years so long as
the patented item (human drug product, animal drug product, medical
device, food additive, or color additive) was subject to regulatory
review by FDA before the item was marketed. Under these acts, a
product's regulatory review period forms the basis for determining the
amount of extension an applicant may receive.
A regulatory review period consists of two periods of time: A
testing phase and an approval phase. For human biological products, the
testing phase begins when the exemption to permit the clinical
investigations of the biological becomes effective and runs until the
approval phase begins. The approval phase starts with the initial
submission of an application to market the human biological product and
continues until FDA grants permission to market the biological product.
Although only a portion of a regulatory review period may count toward
the actual amount of extension that the Director of Patents and
Trademarks may award (for example, half the testing phase must be
subtracted as well as any time that may have occurred before the patent
was issued), FDA's determination of the length of a regulatory review
period for a human biological product will include all of the testing
phase and approval phase as specified in 35 U.S.C. 156(g)(1)(B).
FDA recently approved for marketing the human biologic product
ATRYN (antithrombin (recombinant)). ATRYN is indicated for the
prevention of peri-operative and peri-partum thromboembolic events in
hereditary antithrombin deficient patients. Subsequent to this
approval, the Patent and Trademark Office received a patent term
restoration application for ATRYN (U.S. Patent No. 6,441,145) from GTC
Biotherapeutics, Inc., and the Patent and Trademark Office requested
FDA's assistance in determining this patent's eligibility for patent
term restoration. In a letter dated February 17, 2010, FDA advised the
Patent and Trademark Office that this human biological product had
undergone a regulatory review period and that the approval of ATRYN
represented the first permitted commercial marketing or use of the
recombinant product. Thereafter, the Patent and Trademark Office
requested that FDA determine the product's regulatory review period.
FDA has determined that the applicable regulatory review period for
ATRYN is 4,468 days. Of this time, 4,285 days occurred during the
testing phase of the regulatory review period, while 183 days occurred
during the approval phase. These periods of time were derived from the
following dates:
1. The date an exemption under section 505(i) of the Federal Food,
Drug, and Cosmetic Act (21 U.S.C. 355(i)) became effective: November
15, 1996. The applicant claims November 14, 1996, as the date the
investigational new drug application (IND) became effective. However,
FDA records indicate that the IND effective date was November 15, 1996,
which was 30 days after FDA receipt of the IND.
2. The date the application was initially submitted with respect to
the human biological product under section 351 of the Public Health
Service Act (42 U.S.C. 262): August 8, 2008. The applicant claims
January 31, 2008, as the date the biologics license application (BLA)
for ATRYN (BLA 125284) was initially submitted. However, FDA records
indicate that BLA 125284 was submitted on August 8, 2008.
3. The date the application was approved: February 6, 2009. FDA has
verified the applicant's claim that BLA 125284 was approved on February
6, 2009.
This determination of the regulatory review period establishes the
maximum potential length of a patent extension. However, the U.S.
Patent and Trademark Office applies several statutory limitations in
its calculations of the actual period for patent extension. In its
application for patent extension, this applicant seeks 1,243 days of
patent term extension.
Anyone with knowledge that any of the dates as published are
incorrect may submit to the Division of Dockets Management (see
ADDRESSES) either electronic or written comments and ask for a
redetermination by May 20, 2011. Furthermore, any interested person may
petition FDA for a determination regarding whether the applicant for
extension acted with due diligence during the regulatory review period
by September 19, 2011. To meet its burden, the petition must contain
sufficient facts to merit an FDA investigation. (See H. Rept. 857, part
1, 98th Cong., 2d sess., pp. 41-42, 1984.) Petitions should be in the
format specified in 21 CFR 10.30.
Interested persons may submit to the Division of Dockets Management
(see ADDRESSES) electronic or written comments and written petitions.
It is only necessary to send one set of comments. It is no longer
necessary to send three copies of mailed comments. However, if you
submit a written petition, you must submit three copies of the
petition. Identify comments with
[[Page 15324]]
the docket number found in brackets in the heading of this document.
Comments and petitions that have not been made publicly available
on https://www.regulations.gov may be viewed in the Division of Dockets
Management between 9 a.m. and 4 p.m., Monday through Friday.
Dated: February 14, 2011.
Jane A. Axelrad,
Associate Director for Policy, Center for Drug Evaluation and Research.
[FR Doc. 2011-6509 Filed 3-18-11; 8:45 am]
BILLING CODE P
