Determination That the OXYCONTIN (Oxycodone Hydrochloride) Drug Products Covered by New Drug Application 20-553 Were Withdrawn From Sale for Reasons of Safety or Effectiveness, 23273-23275 [2013-09092]
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Federal Register / Vol. 78, No. 75 / Thursday, April 18, 2013 / Notices
states that ‘‘The public disclosure of
information originally supplied by the
Federal government to the recipient for
the purpose of disclosure to the public
is not included * * *’’ within the
definition of ‘‘collection of
information.’’
FDA requests public comments on the
information collection provisions
described in this document and set forth
in the following table:
TABLE 1—ESTIMATED ANNUAL REPORTING BURDEN 1
Number of
responses per
respondent
Number of
respondents
Activity
Total annual
responses
Average
burden per
response
Total hours
Submission to Docket Number FDA–2008–D–0150 ...........
Cardiovascular Outcome Claim Supplement Submission ...
1
8
1
2.5
1
20
10
20
10
400
Total ..............................................................................
........................
........................
........................
........................
410
1 There
are no capital costs or operating and maintenance costs associated with this collection of information.
Dated: April 12, 2013.
Leslie Kux,
Assistant Commissioner for Policy.
[FR Doc. 2013–09093 Filed 4–17–13; 8:45 am]
BILLING CODE 4160–01–P
DEPARTMENT OF HEALTH AND
HUMAN SERVICES
Food and Drug Administration
[Docket Nos. FDA–2001–P–0238, FDA–
2010–P–0526, FDA–2010–P–0540, FDA–
2011–P–0473]
Determination That the OXYCONTIN
(Oxycodone Hydrochloride) Drug
Products Covered by New Drug
Application 20–553 Were Withdrawn
From Sale for Reasons of Safety or
Effectiveness
AGENCY:
Food and Drug Administration,
HHS.
ACTION:
Notice.
The Food and Drug
Administration (FDA) has determined
that OXYCONTIN (oxycodone
hydrochloride) extended-release tablets
(10 milligrams (mg), 15 mg, 20 mg, 30
mg, 40 mg, 60 mg, 80 mg, and 160 mg)
approved under new drug application
(NDA) 20–553 were withdrawn from
sale for reasons of safety or
effectiveness. The Agency will not
accept or approve abbreviated new drug
applications (ANDAs) for products that
reference NDA 20–553.
FOR FURTHER INFORMATION CONTACT:
Patrick Raulerson, Center for Drug
Evaluation and Research, Food and
Drug Administration, 10903 New
Hampshire Ave., Bldg. 51, Rm. 6368,
Silver Spring, MD 20993–0002, 301–
796–3522.
SUPPLEMENTARY INFORMATION:
sroberts on DSK5SPTVN1PROD with NOTICES
SUMMARY:
I. Background
In 1984, Congress enacted the Drug
Price Competition and Patent Term
Restoration Act of 1984 (Pub. L. 98–417)
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(the 1984 amendments), which
authorized the approval of duplicate
versions of drug products under an
ANDA procedure. ANDA applicants
must, with certain exceptions, show that
the drug for which they are seeking
approval contains the same active
ingredient in the same strength and
dosage form as the ‘‘listed drug,’’ which
is a version of the drug that was
previously approved. ANDA applicants
do not have to repeat the extensive
clinical testing otherwise necessary to
gain approval of a new drug application
(NDA).
The 1984 amendments include what
is now section 505(j)(7) of the Federal
Food, Drug, and Cosmetic Act (21 U.S.C.
355(j)(7)), which requires FDA to
publish a list of all approved drugs.
FDA publishes this list as part of the
‘‘Approved Drug Products With
Therapeutic Equivalence Evaluations,’’
which is known generally as the
‘‘Orange Book.’’ Under FDA regulations,
drugs are removed from the list if the
Agency withdraws or suspends
approval of the drug’s NDA or ANDA
for reasons of safety or effectiveness or
if FDA determines that the listed drug
was withdrawn from sale for reasons of
safety or effectiveness (21 U.S.C.
355(j)(7)(C); 21 CFR 314.162).
A person may petition the Agency to
determine, or the Agency may
determine on its own initiative, whether
a listed drug was withdrawn from sale
for reasons of safety or effectiveness.
This determination may be made at any
time after the drug has been withdrawn
from sale, but must be made before
approving an ANDA that refers to the
listed drug (§ 314.161 (21 CFR 314.161)).
FDA may not approve an ANDA that
does not refer to a listed drug.
OXYCONTIN (oxycodone
hydrochloride) extended-release tablets,
10 mg, 15 mg, 20 mg, 30 mg, 40 mg, 60
mg, 80 mg, and 160 mg (original
OxyContin), are the subject of NDA 20–
553, held by Purdue Pharma LP
(Purdue) and initially approved on
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December 12, 1995. A reformulated
version of these products, OXYCONTIN
(oxycodone hydrochloride) extendedrelease tablets, 10 mg, 15 mg, 20 mg, 30
mg, 40 mg, 60 mg, and 80 mg
(reformulated OxyContin), are the
subject of NDA 22–272, also held by
Purdue and initially approved on April
5, 2010. Reformulated OxyContin was
developed with physicochemical
properties that are intended to make the
tablet more difficult to manipulate for
purposes of abuse or misuse. Both
original and reformulated OxyContin
are opioid agonist products indicated
for the management of moderate to
severe pain when a continuous, aroundthe-clock opioid analgesic is needed for
an extended period of time.
In correspondence dated August 10,
2010, Purdue notified FDA that it had
ceased shipment of original OxyContin,
and FDA subsequently moved original
OxyContin to the ‘‘Discontinued Drug
Product List’’ section of the Orange
Book. On April 16, 2013, FDA approved
a supplemental application for
reformulated OxyContin, approving
changes to the product labeling that
describe certain abuse-deterrent
properties of the reformulated product.
Several parties have submitted citizen
petitions under 21 CFR 10.30,
requesting that the Agency determine
whether original OXYCONTIN
(oxycodone hydrochloride) extendedrelease tablets were voluntarily
withdrawn from sale for reasons other
than safety or effectiveness.1
Based on the information available at
this time, FDA has determined under
§ 314.161 that original OxyContin was
1 Varam, Inc., Docket No. 2011–P–0473 (June 9,
2011) (10, 15, 20, 30, 40, 50, 80, and 160 mg);
Sheppard, Mullin, Richter & Hampton LLP, Docket
No. 2010–P–0540 (Oct. 8, 2010) (10, 15, 20, 30, 40,
60, and 80 mg); Lachman Consultant Services, Inc.,
Docket No. FDA–2010–P–0526) (Sept. 30, 2010) (10,
15, 20, 30, 40, 60, 80, and 160 mg). Lachman also
submitted a petition in 2001 concerning just
Purdue’s 2001 withdrawal of the 160 mg strength.
Docket No. FDA–2001–P–0473 (formerly Docket
No. 2001P–0426) (Sept. 18, 2001).
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Federal Register / Vol. 78, No. 75 / Thursday, April 18, 2013 / Notices
sroberts on DSK5SPTVN1PROD with NOTICES
withdrawn from sale for reasons of
safety or effectiveness. FDA has reached
this determination following a careful
review and analysis of the following
information: (1) The citizen petitions
described previously; (2) the comments
submitted to the dockets associated with
these petitions; (3) the Agency records
and other information concerning
original and reformulated OxyContin
and the withdrawal of original
OxyContin; and (d) data, literature, and
other information concerning
postmarketing adverse events associated
with original OxyContin, reformulated
OxyContin, and other extended-release
oxycodone products.
II. Initiatives To Address Abuse of
Opioid Analgesics
Opioid analgesics are an important
component of modern pain
management. Abuse and misuse of these
products, however, has grown into a
public health epidemic. According to
the Centers for Disease Control and
Prevention, sales of prescription opioids
in the United States increased over 300
percent from 1999 to 2008 (Ref. 1).
Overdose deaths involving these
products increased commensurately
over the same period, from 4,000 to
14,800 (Refs. 1 and 2). In 2008
prescription opioids were involved in
more overdose deaths than heroin and
cocaine combined (Ref. 3). In 2010 the
number of overdose deaths in which
prescription opioids were involved rose
to 16,651, which represented more than
75 percent of all overdose deaths
involving prescription drugs (Ref. 4).
FDA, together with other Federal
agencies, is working to address this
large and growing problem while
ensuring that patients in pain have
appropriate access to opioid analgesics.
FDA has worked to improve the labeling
of OxyContin and other opioid
analgesics to better warn prescribers and
patients of the serious risks associated
with abuse and misuse. FDA also has
worked extensively with the sponsors of
OxyContin and other extended-release
or long-acting prescription (ER/LA)
opioid analgesics to address these risks
through a classwide risk evaluation and
mitigation strategy (REMS) https://
www.fda.gov/downloads/Drugs/
DrugSafety/PostmarketDrug
SafetyInformationfor
PatientsandProviders/UCM311290.pdf.
This REMS, approved on July 9, 2012,
requires sponsors of ER/LA opioids to
make available training for health care
professionals on proper prescribing
practices and also to distribute
educational materials to prescribers and
patients on the safe use of these
medications.
FDA considers the development of
opioid analgesics that can deter abuse
and misuse to be a public health
priority. Opioid analgesics can be
abused orally or by injection, snorting,
or smoking and also may be misused in
therapeutic contexts. Products may be
designed to deter one or more of these
methods of abuse or misuse. Following
mandates in the 2011 White House
prescription drug abuse prevention plan
(Ref. 5) and section 1122(c) of the Food
and Drug Administration Safety and
Innovation Act (Pub. L. 112–144) (126
Stat. 1075), FDA recently issued a draft
guidance to industry on the evaluation
and labeling of potentially abusedeterrent opioid analgesics (Ref. 6).
III. Assessment of Abuse-Deterrent
Properties of Reformulated OxyContin
All forms of opioid analgesic abuse
are dangerous, and non-oral routes of
abuse are particularly dangerous.
Intranasal and intravenous opioid abuse
is associated with serious adverse
events including addiction, overdose,
and death (Refs. 7, 8, and 9).
Intravenous opioid abuse is associated
with HIV and hepatitis B and C
infection risk (Ref. 10). Further, as
stated in the OxyContin labeling (see
section 9.2), injection of OxyContin
excipients ‘‘can result in death, local
tissue necrosis, infection, pulmonary
granulomas, and increased risk of
endocarditis and valvular heart injury.’’
The label is available at https://
www.accessdata.fda.gov/drugsatfda_
docs/label/2013/022272s016lbl.pdf.
Intranasal opioid abuse is associated
with nasal, palatal, and pharyngeal
necrosis (Refs. 7 and 11).
Original OxyContin was often abused
by manipulating the product to defeat
its extended-release mechanism,
causing the oxycodone to be released
more rapidly. Original OxyContin also
was manipulated for therapeutic
purposes, for example, by crushing the
product to sprinkle it onto food or to
administer it through a gastric tube. As
noted in the boxed warning of the
labeling, disruption of the tablet and
controlled-release mechanism for abuse
or misuse ‘‘can lead to rapid release and
absorption of a potentially fatal dose of
oxycodone.’’
FDA has conducted an extensive
review of data available to the Agency
regarding reformulated OxyContin,
including in vitro, pharmacokinetic,
clinical abuse potential, and
postmarketing study data. The data
show that, when compared to original
OxyContin, reformulated OxyContin has
an increased ability to resist crushing,
breaking, and dissolution using a variety
of tools and solvents. The data also
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demonstrate that, when subjected to an
aqueous environment, reformulated
OxyContin gradually forms a viscous
hydrogel. The data also indicate that
insufflation of finely crushed
reformulated OxyContin was associated
with lower ‘‘liking’’ compared to finely
crushed original OxyContin in
recreational opioid users with a history
of intranasal drug abuse. FDA
concludes, based on these data and our
review of all data and information
available to the Agency at this time, that
the physicochemical properties of
reformulated OxyContin are expected to
make abuse via injection difficult and
are expected to reduce abuse via the
intranasal route. In addition,
reformulated OxyContin also may deter
certain types of misuse in therapeutic
contexts.
Additional postmarketing studies
intended to assess the impact of
reformulated OxyContin on abuse and
misuse in the community also have
been conducted; some of these are still
ongoing. FDA has reviewed the
available data from these studies and
has concluded that they suggest, but do
not confirm, a reduction in non-oral
abuse. The Agency will continue to
review data from these studies as they
become available, as well as any other
relevant data that may be developed in
the future.
FDA has long considered the abuse
potential of a drug in numerous
regulatory contexts. Where appropriate,
FDA may take into account abuse
potential as part of the safety profile of
a drug when weighing its benefits and
risks. In this case, FDA has considered
the abuse potential as part of the
Agency’s determination of whether the
original formulation of OxyContin was
withdrawn from sale for reasons of
safety or effectiveness. This approach is
particularly appropriate here in light of
the extensive and well-documented
history of OxyContin abuse.
Original OxyContin has the same
therapeutic benefits as reformulated
OxyContin. Original OxyContin,
however, poses an increased potential
for abuse by certain routes of
administration, when compared to
reformulated OxyContin. Based on the
totality of the data and information
available to the Agency at this time,
FDA concludes that the benefits of
original OxyContin no longer outweigh
its risks. FDA has determined that
OXYCONTIN (oxycodone
hydrochloride) extended release tablets,
10 mg, 15 mg, 20 mg, 30 mg, 40 mg, 60
mg, 80 mg, and 160 mg (approved under
new drug application 20–553), were
withdrawn from sale for reasons of
safety or effectiveness. Accordingly, the
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Federal Register / Vol. 78, No. 75 / Thursday, April 18, 2013 / Notices
Agency will remove OXYCONTIN
(oxycodone hydrochloride) extendedrelease tablets (10 mg, 15 mg, 20 mg, 30
mg, 40 mg, 60 mg, 80 mg, and 160 mg)
approved under NDA 20–553 from the
list of drug products published in the
Orange Book. FDA will not accept or
approve ANDAs that refer to these drug
products.
sroberts on DSK5SPTVN1PROD with NOTICES
IV. References
The following references have been
placed on display in the Division of
Dockets Management (HFA–305), Food
and Drug Administration, 5630 Fishers
Lane, Rm. 1061, Rockville, MD 20852,
and may be seen by interested persons
between 9 a.m. and 4 p.m., Monday
through Friday, and are available
electronically at https://
www.regulations.gov. (FDA has verified
the Web site addresses in this reference
section, but FDA is not responsible for
any subsequent changes to the Web sites
after this document publishes in the
Federal Register.)
1. National Center for Injury Prevention and
Control, Centers for Disease Control and
Prevention (CDC), ‘‘Policy Impact:
Prescription Painkiller Overdoses’’
(www.cdc.gov/
HomeandRecreationalSafety/pdf/
PolicyImpact-Prescription
PainkillerOD.pdf).
2. CDC, ‘‘Vital Signs: Overdoses of
Prescription Opioid Pain Relievers—
United States, 1999–2008,’’ Morbidity
and Mortality Weekly Report, vol. 60,
No. 43, pp. 1487–1492, 2011
(www.cdc.gov/mmwr/pdf/wk/
mm6043.pdf).
3. National Center for Injury Prevention and
Control, CDC, ‘‘Unintentional Drug
Poisoning in the United States’’
(www.cdc.gov/HomeandRecreational
Safety/pdf/poison-issue-brief.pdf).
4. Jones, C.M., K.A. Mack, and L.J. Paulozzi,
‘‘Pharmaceutical Overdose Deaths,
United States, 2010,’’ Journal of the
American Medical Association, vol. 309,
pp. 657–659, 2013.
5. FDA, ‘‘FDA Blueprint for Prescriber
Education for Extended-Release and
Long-Acting Opioid Analgesics’’ (https://
www.fda.gov/downloads/drugs/
drugsafety/informationbydrugclass/
ucm277916.pdf).
6. FDA, ‘‘Draft Guidance for Industry: AbuseDeterrent Opioids—Evaluation and
Labeling,’’ (www.fda.gov/downloads/
Drugs/GuidanceCompliance
RegulatoryInformation/Guidances/
UCM334743.pdf).
7. Katz, N., R.C. Dart, E. Bailey, et al.,
‘‘Tampering With Prescription Opioids:
Nature and Extent of the Problem, Health
Consequences, and Solutions,’’ The
American Journal of Drug and Alcohol
Abuse, vol. 37, pp. 205–217, 2011.
8. Silva, K., S.M. Schrager, A. Kecojevic, et
al., ‘‘Factors Associated With History of
Non-Fatal Overdose Among Young
Nonmedical Users of Prescription
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Drugs,’’ Drug and Alcohol Dependence,
vol. 128, pp. 104–110, 2013.
9. Degenhardt, L., C. Bucello, B. Mathers, et
al., ‘‘Mortality Among Regular or
Dependent Users of Heroin and Other
Opioids: A Systematic Review and MetaAnalysis of Cohort Studies,’’ Addiction,
vol. 106, pp. 32–51, 2011.
10. CDC, ‘‘Integrated Prevention Services for
HIV Infection, Viral Hepatitis, Sexually
Transmitted Diseases, and Tuberculosis
for Persons Who Use Drugs Illicitly:
Summary Guidance From the CDC and
the U.S. Department of Health and
Human Services,’’ Morbidity and
Mortality Weekly Report, vol. 61, pp. 1–
40, 2012.
11. Alexander, D., K. Alexander, and J.
Valentino, ‘‘Intranasal HydrocodoneAcetaminophen Abuse-Induced Necrosis
of the Nasal Cavity and Pharynx,’’ The
Laryngoscope, vol. 122, pp. 2378–2381,
2012.
Dated: April 12, 2013.
Leslie Kux,
Assistant Commissioner for Policy.
[FR Doc. 2013–09092 Filed 4–16–13; 4:15 pm]
BILLING CODE 4160–01–P
DEPARTMENT OF HEALTH AND
HUMAN SERVICES
Health Resources and Service
Administration
Advisory Committee on
Interdisciplinary, Community-Based
Linkages; Notice of Meeting
In accordance with section 10(a)(2) of
the Federal Advisory Committee Act
(Pub. L. 92–463), notice is hereby given
of the following meeting:
Name: Advisory Committee on
Interdisciplinary, Community-Based
Linkages (ACICBL).
Dates and Times: April 22, 2013, 8:30
a.m.–5:00 p.m., April 23, 2013, 9:00
a.m.–5:00 p.m.
Place: Health Resources and Services
Administration, U.S. Department of
Health and Human Services, 5600
Fishers Lane, Rockville, Maryland
20852, Room 18–57.
Status: The meeting will be open to
the public.
Purpose: The members of the ACICBL
will begin discussions to develop the
legislatively mandated 13th Annual
Report to the Secretary of Health and
Human Services and Congress. The
Committee members will focus on the
working topic: Optimizing the
Interprofessional Team Member’s
Contributions to Population Health. The
Committee has invited Dr. John Gilbert,
former Principal and Professor Emeritus
at the University of British Columbia,
Canada; Ms. Rachel Watman, Senior
Program Officer, The John A. Hartford
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23275
Foundation; Dr. John Bulger, Chief
Quality Officer, Geisinger Health
System; Dr. Paul McGann, Deputy Chief
Medical Officer for Innovation Grants,
Centers for Medicare & Medicaid
Services; Dr. Thomas Edes, Director of
Home and Community-Based Care, U.S.
Department of Veterans Affairs; and Dr.
Alex Camacho, Deputy Director, Office
of Performance Measurement, Health
Resources and Services Administration.
The meeting will afford committee
members with the opportunity to
identify and discuss population health;
interprofessional education, care and
competencies; and best practices and
the like in an effort to formulate
appropriate recommendations for the
Secretary and the Congress.
Agenda: The ACICBL agenda includes
an overview of the Committee’s general
business activities, presentations by and
dialogue with experts, and discussion
sessions specifically for the
development of recommendations to be
addressed in the 13th Annual ACICBL
Report. The agenda will be available 2
days prior to the meeting on the HRSA
Web site (https://www.hrsa.gov/
advisorycommittees/bhpradvisory/
acicbl/acicbl.html). Agenda items are
subject to change as priorities dictate.
Members
of the public and interested parties may
request to provide comments or register
to attend the meeting by emailing their
first name, last name, and full email
address to
BHPRAdvisoryCommittee@hrsa.gov or
by contacting Ms. Crystal Straughn at
301–443–3594. Registration is first
come, first served as space is limited.
SUPPLEMENTARY INFORMATION:
FOR FURTHER INFORMATION CONTACT:
Anyone requesting information
regarding the ACICBL should contact
Dr. Joan Weiss, Designated Federal
Official within the Bureau of Health
Professions, Health Resources and
Services Administration, in one of three
ways: (1) Send a request to the following
address: Dr. Joan Weiss, Designated
Federal Official, Bureau of Health
Professions, Health Resources and
Services Administration, Parklawn
Building, Room 9C–05, 5600 Fishers
Lane, Rockville, Maryland 20857; (2)
call (301) 443–6950; or (3) send an email
to jweiss@hrsa.gov.
Dated: April 11, 2013.
Bahar Niakan,
Director, Division of Policy and Information
Coordination.
[FR Doc. 2013–09135 Filed 4–17–13; 8:45 am]
BILLING CODE 4165–15–P
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]]>Agencies
[Federal Register Volume 78, Number 75 (Thursday, April 18, 2013)]
[Notices]
[Pages 23273-23275]
From the Federal Register Online via the Government Printing Office [www.gpo.gov]
[FR Doc No: 2013-09092]
-----------------------------------------------------------------------
DEPARTMENT OF HEALTH AND HUMAN SERVICES
Food and Drug Administration
[Docket Nos. FDA-2001-P-0238, FDA-2010-P-0526, FDA-2010-P-0540, FDA-
2011-P-0473]
Determination That the OXYCONTIN (Oxycodone Hydrochloride) Drug
Products Covered by New Drug Application 20-553 Were Withdrawn From
Sale for Reasons of Safety or Effectiveness
AGENCY: Food and Drug Administration, HHS.
ACTION: Notice.
-----------------------------------------------------------------------
SUMMARY: The Food and Drug Administration (FDA) has determined that
OXYCONTIN (oxycodone hydrochloride) extended-release tablets (10
milligrams (mg), 15 mg, 20 mg, 30 mg, 40 mg, 60 mg, 80 mg, and 160 mg)
approved under new drug application (NDA) 20-553 were withdrawn from
sale for reasons of safety or effectiveness. The Agency will not accept
or approve abbreviated new drug applications (ANDAs) for products that
reference NDA 20-553.
FOR FURTHER INFORMATION CONTACT: Patrick Raulerson, Center for Drug
Evaluation and Research, Food and Drug Administration, 10903 New
Hampshire Ave., Bldg. 51, Rm. 6368, Silver Spring, MD 20993-0002, 301-
796-3522.
SUPPLEMENTARY INFORMATION:
I. Background
In 1984, Congress enacted the Drug Price Competition and Patent
Term Restoration Act of 1984 (Pub. L. 98-417) (the 1984 amendments),
which authorized the approval of duplicate versions of drug products
under an ANDA procedure. ANDA applicants must, with certain exceptions,
show that the drug for which they are seeking approval contains the
same active ingredient in the same strength and dosage form as the
``listed drug,'' which is a version of the drug that was previously
approved. ANDA applicants do not have to repeat the extensive clinical
testing otherwise necessary to gain approval of a new drug application
(NDA).
The 1984 amendments include what is now section 505(j)(7) of the
Federal Food, Drug, and Cosmetic Act (21 U.S.C. 355(j)(7)), which
requires FDA to publish a list of all approved drugs. FDA publishes
this list as part of the ``Approved Drug Products With Therapeutic
Equivalence Evaluations,'' which is known generally as the ``Orange
Book.'' Under FDA regulations, drugs are removed from the list if the
Agency withdraws or suspends approval of the drug's NDA or ANDA for
reasons of safety or effectiveness or if FDA determines that the listed
drug was withdrawn from sale for reasons of safety or effectiveness (21
U.S.C. 355(j)(7)(C); 21 CFR 314.162).
A person may petition the Agency to determine, or the Agency may
determine on its own initiative, whether a listed drug was withdrawn
from sale for reasons of safety or effectiveness. This determination
may be made at any time after the drug has been withdrawn from sale,
but must be made before approving an ANDA that refers to the listed
drug (Sec. 314.161 (21 CFR 314.161)). FDA may not approve an ANDA that
does not refer to a listed drug.
OXYCONTIN (oxycodone hydrochloride) extended-release tablets, 10
mg, 15 mg, 20 mg, 30 mg, 40 mg, 60 mg, 80 mg, and 160 mg (original
OxyContin), are the subject of NDA 20-553, held by Purdue Pharma LP
(Purdue) and initially approved on December 12, 1995. A reformulated
version of these products, OXYCONTIN (oxycodone hydrochloride)
extended-release tablets, 10 mg, 15 mg, 20 mg, 30 mg, 40 mg, 60 mg, and
80 mg (reformulated OxyContin), are the subject of NDA 22-272, also
held by Purdue and initially approved on April 5, 2010. Reformulated
OxyContin was developed with physicochemical properties that are
intended to make the tablet more difficult to manipulate for purposes
of abuse or misuse. Both original and reformulated OxyContin are opioid
agonist products indicated for the management of moderate to severe
pain when a continuous, around-the-clock opioid analgesic is needed for
an extended period of time.
In correspondence dated August 10, 2010, Purdue notified FDA that
it had ceased shipment of original OxyContin, and FDA subsequently
moved original OxyContin to the ``Discontinued Drug Product List''
section of the Orange Book. On April 16, 2013, FDA approved a
supplemental application for reformulated OxyContin, approving changes
to the product labeling that describe certain abuse-deterrent
properties of the reformulated product.
Several parties have submitted citizen petitions under 21 CFR
10.30, requesting that the Agency determine whether original OXYCONTIN
(oxycodone hydrochloride) extended-release tablets were voluntarily
withdrawn from sale for reasons other than safety or effectiveness.\1\
---------------------------------------------------------------------------
\1\ Varam, Inc., Docket No. 2011-P-0473 (June 9, 2011) (10, 15,
20, 30, 40, 50, 80, and 160 mg); Sheppard, Mullin, Richter & Hampton
LLP, Docket No. 2010-P-0540 (Oct. 8, 2010) (10, 15, 20, 30, 40, 60,
and 80 mg); Lachman Consultant Services, Inc., Docket No. FDA-2010-
P-0526) (Sept. 30, 2010) (10, 15, 20, 30, 40, 60, 80, and 160 mg).
Lachman also submitted a petition in 2001 concerning just Purdue's
2001 withdrawal of the 160 mg strength. Docket No. FDA-2001-P-0473
(formerly Docket No. 2001P-0426) (Sept. 18, 2001).
---------------------------------------------------------------------------
Based on the information available at this time, FDA has determined
under Sec. 314.161 that original OxyContin was
[[Page 23274]]
withdrawn from sale for reasons of safety or effectiveness. FDA has
reached this determination following a careful review and analysis of
the following information: (1) The citizen petitions described
previously; (2) the comments submitted to the dockets associated with
these petitions; (3) the Agency records and other information
concerning original and reformulated OxyContin and the withdrawal of
original OxyContin; and (d) data, literature, and other information
concerning postmarketing adverse events associated with original
OxyContin, reformulated OxyContin, and other extended-release oxycodone
products.
II. Initiatives To Address Abuse of Opioid Analgesics
Opioid analgesics are an important component of modern pain
management. Abuse and misuse of these products, however, has grown into
a public health epidemic. According to the Centers for Disease Control
and Prevention, sales of prescription opioids in the United States
increased over 300 percent from 1999 to 2008 (Ref. 1). Overdose deaths
involving these products increased commensurately over the same period,
from 4,000 to 14,800 (Refs. 1 and 2). In 2008 prescription opioids were
involved in more overdose deaths than heroin and cocaine combined (Ref.
3). In 2010 the number of overdose deaths in which prescription opioids
were involved rose to 16,651, which represented more than 75 percent of
all overdose deaths involving prescription drugs (Ref. 4).
FDA, together with other Federal agencies, is working to address
this large and growing problem while ensuring that patients in pain
have appropriate access to opioid analgesics. FDA has worked to improve
the labeling of OxyContin and other opioid analgesics to better warn
prescribers and patients of the serious risks associated with abuse and
misuse. FDA also has worked extensively with the sponsors of OxyContin
and other extended-release or long-acting prescription (ER/LA) opioid
analgesics to address these risks through a classwide risk evaluation
and mitigation strategy (REMS) https://www.fda.gov/downloads/Drugs/DrugSafety/PostmarketDrugSafetyInformationforPatientsandProviders/UCM311290.pdf.
This REMS, approved on July 9, 2012, requires sponsors of ER/LA
opioids to make available training for health care professionals on
proper prescribing practices and also to distribute educational
materials to prescribers and patients on the safe use of these
medications.
FDA considers the development of opioid analgesics that can deter
abuse and misuse to be a public health priority. Opioid analgesics can
be abused orally or by injection, snorting, or smoking and also may be
misused in therapeutic contexts. Products may be designed to deter one
or more of these methods of abuse or misuse. Following mandates in the
2011 White House prescription drug abuse prevention plan (Ref. 5) and
section 1122(c) of the Food and Drug Administration Safety and
Innovation Act (Pub. L. 112-144) (126 Stat. 1075), FDA recently issued
a draft guidance to industry on the evaluation and labeling of
potentially abuse-deterrent opioid analgesics (Ref. 6).
III. Assessment of Abuse-Deterrent Properties of Reformulated OxyContin
All forms of opioid analgesic abuse are dangerous, and non-oral
routes of abuse are particularly dangerous. Intranasal and intravenous
opioid abuse is associated with serious adverse events including
addiction, overdose, and death (Refs. 7, 8, and 9). Intravenous opioid
abuse is associated with HIV and hepatitis B and C infection risk (Ref.
10). Further, as stated in the OxyContin labeling (see section 9.2),
injection of OxyContin excipients ``can result in death, local tissue
necrosis, infection, pulmonary granulomas, and increased risk of
endocarditis and valvular heart injury.'' The label is available at
https://www.accessdata.fda.gov/drugsatfda_docs/label/2013/022272s016lbl.pdf. Intranasal opioid abuse is associated with nasal,
palatal, and pharyngeal necrosis (Refs. 7 and 11).
Original OxyContin was often abused by manipulating the product to
defeat its extended-release mechanism, causing the oxycodone to be
released more rapidly. Original OxyContin also was manipulated for
therapeutic purposes, for example, by crushing the product to sprinkle
it onto food or to administer it through a gastric tube. As noted in
the boxed warning of the labeling, disruption of the tablet and
controlled-release mechanism for abuse or misuse ``can lead to rapid
release and absorption of a potentially fatal dose of oxycodone.''
FDA has conducted an extensive review of data available to the
Agency regarding reformulated OxyContin, including in vitro,
pharmacokinetic, clinical abuse potential, and postmarketing study
data. The data show that, when compared to original OxyContin,
reformulated OxyContin has an increased ability to resist crushing,
breaking, and dissolution using a variety of tools and solvents. The
data also demonstrate that, when subjected to an aqueous environment,
reformulated OxyContin gradually forms a viscous hydrogel. The data
also indicate that insufflation of finely crushed reformulated
OxyContin was associated with lower ``liking'' compared to finely
crushed original OxyContin in recreational opioid users with a history
of intranasal drug abuse. FDA concludes, based on these data and our
review of all data and information available to the Agency at this
time, that the physicochemical properties of reformulated OxyContin are
expected to make abuse via injection difficult and are expected to
reduce abuse via the intranasal route. In addition, reformulated
OxyContin also may deter certain types of misuse in therapeutic
contexts.
Additional postmarketing studies intended to assess the impact of
reformulated OxyContin on abuse and misuse in the community also have
been conducted; some of these are still ongoing. FDA has reviewed the
available data from these studies and has concluded that they suggest,
but do not confirm, a reduction in non-oral abuse. The Agency will
continue to review data from these studies as they become available, as
well as any other relevant data that may be developed in the future.
FDA has long considered the abuse potential of a drug in numerous
regulatory contexts. Where appropriate, FDA may take into account abuse
potential as part of the safety profile of a drug when weighing its
benefits and risks. In this case, FDA has considered the abuse
potential as part of the Agency's determination of whether the original
formulation of OxyContin was withdrawn from sale for reasons of safety
or effectiveness. This approach is particularly appropriate here in
light of the extensive and well-documented history of OxyContin abuse.
Original OxyContin has the same therapeutic benefits as
reformulated OxyContin. Original OxyContin, however, poses an increased
potential for abuse by certain routes of administration, when compared
to reformulated OxyContin. Based on the totality of the data and
information available to the Agency at this time, FDA concludes that
the benefits of original OxyContin no longer outweigh its risks. FDA
has determined that OXYCONTIN (oxycodone hydrochloride) extended
release tablets, 10 mg, 15 mg, 20 mg, 30 mg, 40 mg, 60 mg, 80 mg, and
160 mg (approved under new drug application 20-553), were withdrawn
from sale for reasons of safety or effectiveness. Accordingly, the
[[Page 23275]]
Agency will remove OXYCONTIN (oxycodone hydrochloride) extended-release
tablets (10 mg, 15 mg, 20 mg, 30 mg, 40 mg, 60 mg, 80 mg, and 160 mg)
approved under NDA 20-553 from the list of drug products published in
the Orange Book. FDA will not accept or approve ANDAs that refer to
these drug products.
IV. References
The following references have been placed on display in the
Division of Dockets Management (HFA-305), Food and Drug Administration,
5630 Fishers Lane, Rm. 1061, Rockville, MD 20852, and may be seen by
interested persons between 9 a.m. and 4 p.m., Monday through Friday,
and are available electronically at https://www.regulations.gov. (FDA
has verified the Web site addresses in this reference section, but FDA
is not responsible for any subsequent changes to the Web sites after
this document publishes in the Federal Register.)
1. National Center for Injury Prevention and Control, Centers for
Disease Control and Prevention (CDC), ``Policy Impact: Prescription
Painkiller Overdoses'' (www.cdc.gov/HomeandRecreationalSafety/pdf/PolicyImpact-PrescriptionPainkillerOD.pdf).
2. CDC, ``Vital Signs: Overdoses of Prescription Opioid Pain
Relievers--United States, 1999-2008,'' Morbidity and Mortality
Weekly Report, vol. 60, No. 43, pp. 1487-1492, 2011 (www.cdc.gov/mmwr/pdf/wk/mm6043.pdf).
3. National Center for Injury Prevention and Control, CDC,
``Unintentional Drug Poisoning in the United States'' (www.cdc.gov/HomeandRecreationalSafety/pdf/poison-issue-brief.pdf).
4. Jones, C.M., K.A. Mack, and L.J. Paulozzi, ``Pharmaceutical
Overdose Deaths, United States, 2010,'' Journal of the American
Medical Association, vol. 309, pp. 657-659, 2013.
5. FDA, ``FDA Blueprint for Prescriber Education for Extended-
Release and Long-Acting Opioid Analgesics'' (https://www.fda.gov/downloads/drugs/drugsafety/informationbydrugclass/ucm277916.pdf).
6. FDA, ``Draft Guidance for Industry: Abuse-Deterrent Opioids--
Evaluation and Labeling,'' (www.fda.gov/downloads/Drugs/GuidanceComplianceRegulatoryInformation/Guidances/UCM334743.pdf).
7. Katz, N., R.C. Dart, E. Bailey, et al., ``Tampering With
Prescription Opioids: Nature and Extent of the Problem, Health
Consequences, and Solutions,'' The American Journal of Drug and
Alcohol Abuse, vol. 37, pp. 205-217, 2011.
8. Silva, K., S.M. Schrager, A. Kecojevic, et al., ``Factors
Associated With History of Non-Fatal Overdose Among Young Nonmedical
Users of Prescription Drugs,'' Drug and Alcohol Dependence, vol.
128, pp. 104-110, 2013.
9. Degenhardt, L., C. Bucello, B. Mathers, et al., ``Mortality Among
Regular or Dependent Users of Heroin and Other Opioids: A Systematic
Review and Meta-Analysis of Cohort Studies,'' Addiction, vol. 106,
pp. 32-51, 2011.
10. CDC, ``Integrated Prevention Services for HIV Infection, Viral
Hepatitis, Sexually Transmitted Diseases, and Tuberculosis for
Persons Who Use Drugs Illicitly: Summary Guidance From the CDC and
the U.S. Department of Health and Human Services,'' Morbidity and
Mortality Weekly Report, vol. 61, pp. 1-40, 2012.
11. Alexander, D., K. Alexander, and J. Valentino, ``Intranasal
Hydrocodone-Acetaminophen Abuse-Induced Necrosis of the Nasal Cavity
and Pharynx,'' The Laryngoscope, vol. 122, pp. 2378-2381, 2012.
Dated: April 12, 2013.
Leslie Kux,
Assistant Commissioner for Policy.
[FR Doc. 2013-09092 Filed 4-16-13; 4:15 pm]
BILLING CODE 4160-01-P
