Confidentiality of Interim Results in Cardiovascular Outcome Safety Trials; Public Hearing; Request for Comments, 41149-41152 [2014-16374]
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Federal Register / Vol. 79, No. 135 / Tuesday, July 15, 2014 / Proposed Rules
prescribing regulations to assign the use
of the airspace necessary to ensure the
safety of aircraft and the efficient use of
airspace. This regulation is within the
scope of that authority as it would
amend controlled airspace at Charles M.
Schultz-Sonoma County Airport, Santa
Rosa, CA.
This proposal will be subject to an
environmental analysis in accordance
with FAA Order 1050.1E,
‘‘Environmental Impacts: Policies and
Procedures’’ prior to any FAA final
regulatory action.
List of Subjects in 14 CFR Part 71
Airspace, Incorporation by reference,
Navigation (air).
The Proposed Amendment
Accordingly, pursuant to the
authority delegated to me, the Federal
Aviation Administration proposes to
amend 14 CFR Part 71 as follows:
PART 71—DESIGNATION OF CLASS A,
B, C, D AND E AIRSPACE AREAS; AIR
TRAFFIC SERVICE ROUTES; AND
REPORTING POINTS
1. The authority citation for 14 CFR
Part 71 continues to read as follows:
■
Authority: 49 U.S.C. 106(g), 40103, 40113,
40120; E.O. 10854, 24 FR 9565, 3 CFR, 1959–
1963 Comp., p. 389.
§ 71.1
[Amended]
2. The incorporation by reference in
14 CFR 71.1 of the Federal Aviation
Administration Order 7400.9X, Airspace
Designations and Reporting Points,
dated August 7, 2013, and effective
September 15, 2013, is amended as
follows:
■
Paragraph 5000
Class D Airspace
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*
*
*
sroberts on DSK5SPTVN1PROD with PROPOSALS
Paragraph 6004 Class E Airspace Areas
Designated As An Extension to Class D or
Class E Surface Area
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AWP CA E4 Santa Rosa, CA [New]
Charles M. Shultz-Sonoma County Airport,
CA
(Lat. 38°30′33″ N., long. 122°48′46″ W.)
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Paragraph 6005 Class E Airspace Areas
Extending Upward From 700 Feet or More
Above the Surface of the Earth
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AWP CA E5 Santa Rosa, CA [Modified]
Charles M. Shultz-Sonoma County Airport,
CA
(Lat. 38°30′33″ N., long. 122°48′46″ W.)
That airspace extending upward from 700
feet above the surface bounded by a line
beginning at lat. 38°53′25″ N., long.
122°52′34″ W.; to lat. 38°37′07″ N., long. 122°
46′02.00″ W.; to 38°22′08″ N., long.
122°38′28″ W.; lat. 38°06′41″ N., long.
122°29′59″ W.; lat. 38°02′10″ N., long.
122°44′09″ W.; lat. 38°17′57″ N., long.
122°54′37″ W.; lat. 38°22′58″ N., long.
123°02′34″ W.; lat. 38°29′12″ N., long.
122°56′32″ W.; lat. 38°33′48″ N., long.
123°00′47″ W.; lat. 38°50′14″ N., long.
123°07′20″ W. thence to the point of origin;
that airspace extending upward from 1,200
feet above the surface bounded by a line
beginning at lat. 45°49′00″ N., long.
118°00′00″ W.; to lat. 45°49′00″ N., long.
119°45′00″ W.; to lat. 47°00′00″ N., long.
119°45′00″ W., to lat. 47°00′00″ N., long.
118°00′00″ W.; thence to the point of origin.
Issued in Seattle, Washington, on July 2,
2014.
Clark Desing,
Manager, Operations Support Group, Western
Service Center.
[FR Doc. 2014–16636 Filed 7–14–14; 8:45 am]
BILLING CODE 4910–13–P
DEPARTMENT OF HEALTH AND
HUMAN SERVICES
Food and Drug Administration
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AWP CA D Santa Rosa, CA [Amended]
Charles M. Schultz-Sonoma County Airport,
CA
(Lat. 38°30′33″ N., long. 122°48′46″ W.)
That airspace extending upward from the
surface to and including 2,600 feet MSL
within a 4.3-mile radius of Santa Rosa/
Sonoma County Airport. This Class D
airspace area is effective during the specific
dates and times established in advance by a
Notice to Airmen. The effective date and time
will thereafter be continuously published in
the Airport/Facility Directory.
*
That airspace extending upward from the
surface within 2 miles either side of the 342°
bearing from the Charles M. Shultz-Sonoma
County Airport, CA, extending from the 4.3
mile radius of the airport to 14 miles
northwest of the airport.
21 CFR Part 15
[Docket No. FDA–2014–N–0824]
Confidentiality of Interim Results in
Cardiovascular Outcome Safety Trials;
Public Hearing; Request for Comments
AGENCY:
Food and Drug Administration,
41149
researchers, health care providers,
representatives from the pharmaceutical
industry and health care organizations,
and the general public, about
appropriate handling of interim analysis
results of these ongoing CVOTs. FDA is
also opening a public docket to receive
comments on this topic.
DATES: The public hearing will be held
on August 11, 2014, from 8 a.m. to 5
p.m. Individuals who wish to present at
the public hearing must register by July
28, 2014. Section IV provides
attendance and registration information.
To ensure consideration, submit
comments by July 28, 2014. Electronic
or written comments will be accepted
after the public hearing until October
10, 2014.
ADDRESSES: The public hearing will be
held at the FDA White Oak Campus,
10903 New Hampshire Ave., Bldg. 31
Conference Center, the Great Room (rm.
1503), Silver Spring, MD 20993–0002.
Entrance for the public hearing
participants (non-FDA employees) is
through Building 1 where routine
security check procedures will be
performed. For parking and security
information, please refer to https://www.
fda.gov/AboutFDA/WorkingatFDA/
BuildingsandFacilities/WhiteOak
CampusInformation/ucm241740.htm.
Submit electronic comments to https://
www.regulations.gov. Submit written
comments to the Division of Dockets
Management (HFA–305), Food and Drug
Administration, 5630 Fishers Lane, rm.
1061, Rockville, MD 20852. Identify
comments with the docket number
found in brackets in the heading of this
document.
FOR FURTHER INFORMATION CONTACT:
Indira Hills, Food and Drug
Administration, Center for Drug
Evaluation and Research, 10903 New
Hampshire Ave., Bldg. 21, rm. 4508,
Silver Spring, MD 20993, 301–796–
9686, FAX: 301–796–9907, email:
indira.hills@fda.hhs.gov.
SUPPLEMENTARY INFORMATION:
I. Background
ACTION:
A. The Requirement for Postmarketing
Studies To Assess the Risk of a New
Drug
The Food and Drug
Administration (FDA) is announcing a
public hearing that will provide a forum
to discuss confidentiality of interim
results for certain cardiovascular
outcomes trials (CVOTs) submitted to
the Agency while the trials are still
ongoing. The purpose of the public
hearing is to initiate constructive
discussion among regulators,
In some cases, studies submitted to
FDA as part of a new drug application
or biologics license application will
demonstrate that a drug is safe and
effective for its intended use (i.e., that
its benefits outweigh its identified
risks), but the Agency will nevertheless
require a sponsor to conduct additional
postmarketing studies or trials under
section 505(o)(3) of the Federal Food,
Drug, and Cosmetic Act (the FD&C Act)
HHS.
Notification of public hearing;
request for comments.
SUMMARY:
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(21 U.S.C. 355(o)(3)) for the following
reasons: To assess a known serious risk
related to use of the drug, to assess
signals of a serious risk related to use of
the drug, or to identify an unexpected
risk when available data indicate the
potential for a serious risk.
B. FDA’s Approach to the Approval of
Drugs To Treat Type II Diabetes
For most drugs, clinical trials of
reasonable size can establish a favorable
relationship of benefit to relatively
common risks, but they are not large
enough to assess the risk of rare serious
events such as heart attacks, strokes, or
death. Where there is concern about
these risks (e.g., concern about drugs to
treat Type II diabetes mellitus (T2DM)
or to promote weight loss), development
programs include CVOTs to help assess
the risk to meet the requirements for
drug approval. In some cases, applicants
have conducted a metaanalysis of
cardiovascular (CV) risk from Phase 2/
3 trials to help establish the safety of a
drug and a separate larger CVOT as a
postmarketing requirement under
section 505(o)(3) of the FD&C Act. In
other cases, analyses of interim data
from a single CVOT will demonstrate
that a drug is safe with regard to CV risk
for its intended use, and, if the overall
risk-benefit analysis supports approval,
the applicant will further assess the CV
risks by continuing the trial as a
postmarketing requirement.
The Agency has described its
expectations for CV outcome data for
drugs to treat T2DM in the guidance for
industry ‘‘Diabetes Mellitus Evaluating
Cardiovascular Risk in New
Antidiabetic Therapies to Treat Type 2’’
(available at Diabetes’’ (https://www.fda.
gov/downloads/Drugs/Guidance
ComplianceRegulatoryInformation/
Guidances/UCM071627.pdf), which was
issued based on the discussion at an
advisory committee meeting,1 as well as
in other available data and information.
The guidance makes recommendations
about how to demonstrate that a new
therapy to treat T2DM is not associated
with an unacceptable increase in CV
risk.
The guidance states that before
submission of a new drug application
(NDA) or biologics license application,
the premarketing CV outcome data
should show that the incidence of
important CV events occurring with the
investigational agent is not more than 80
percent increase compared to the
control group (i.e., that the upper bound
1 On July 1 and 2, 2008, the Endocrinologic and
Metabolic Drug Advisory Committee met to discuss
the role of CV assessment in the premarketing and
postmarketing settings (https://www.fda.gov/ohrms/
dockets/ac/cder08.html#endocrinologicmetabolic).
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of the 2-sided 95 percent confidence
interval for the estimated risk ratio for
CV events is less than 1.8). The
guidance also states that if the risk ratio
is between 1.3 and 1.8 and the overall
risk-benefit analysis supports approval,
a postmarketing trial will generally be
necessary to show that the upper bound
of the 2-sided 95 percent confidence
interval for the estimated risk ratio is
less than 1.3. This showing can be
achieved by conducting an adequately
powered new postmarketing trial, by
combining results of separate
premarketing and postmarketing trials,
or by continuing a large CVOT in which
a planned interim analysis is the basis
for concluding that the risk ratio is less
than 1.8. If the risk ratio of 1.3 is ruled
out based on premarket data, then a
postmarketing requirement may not be
necessary.
C. Interim Analyses, the Importance of
Their Confidentiality, and the Role of
the Data Monitoring Committee
Interim analyses are analyses of study
data conducted partway through an
ongoing clinical trial. They can play an
integral role in clinical trials by
allowing for the safety of enrolled
patients to be monitored at various
intervals in the study and also by
allowing for the possibility of stopping
the trial early for safety concerns, for
futility, or for early evidence of efficacy
that would make it unethical for the
trial to proceed. Confidentiality of
interim data is a paramount concern:
The 1998 International Conference on
Harmonization (ICH) guidance for
industry ‘‘E9 Statistical Principles for
Clinical Trials’’ (ICH E9 guidance)
(available at https://www.fda.gov/
downloads/Drugs/Guidance
ComplianceRegulatoryInformation/
Guidances/ucm073137.pdf) reflects a
collective view across regulatory
agencies in the European Union, Japan,
and the United States when it states that
‘‘All staff involved in the conduct of the
trial should remain blind to the results
of such analyses, because of the
possibility that their attitudes to the trial
will be modified and cause changes in
the characteristics of patients to be
recruited or biases in treatment
comparisons.’’
An independent Data Monitoring
Committee (DMC) is usually established
to review the interim analysis results
and make recommendations to the
sponsor about any action needed based
on those results, allowing the sponsor
and other personnel associated with the
trial to remain masked to interim
results. In 2006, FDA issued the
guidance for clinical trial sponsors
‘‘Establishment and Operation of
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Clinical Trial Data Monitoring
Committees’’ (DMC guidance) (available
at https://www.fda.gov/downloads/
RegulatoryInformation/Guidances/
UCM127073.pdf) that reiterated many of
the best practices for interim analyses
and DMCs outlined in the ICH E9
guidance. Specifically, the guidance
states that ‘‘[p]rocedures should be
established to safeguard confidential
interim data from the project team,
investigators, sponsor representatives,
or anyone else outside the DMC and the
statistician(s) performing the interim
analyses (see 21 CFR 314.126(b)(5)
(drugs) and 21 CFR 860.7(f)(1)
(devices)).’’ An exception is made in
considering the need to disseminate
safety data to allow for appropriate
monitoring of patients’ safety.
D. Potential Adverse Consequences of
Disclosure of Interim Results
The concern with widespread
disclosure of interim results in an
ongoing trial, as described in the DMC
guidance, stems from the potential of
the disclosure to negatively affect the
conduct of the remaining portion of the
trial. The impact could include
unanticipated changes in recruitment,
treatment administration, or other
aspects of trial conduct, as well as loss
of objectivity in safety event reporting.
Sponsors and other interested parties
with access to interim data may have
difficulty managing the remainder of the
trial in an objective manner, particularly
if changes to the trial protocol are
needed for other reasons. Knowledge of
interim data may influence decisions
about the trial going forward, and it is
nearly impossible to assess the impact
of that influence on the trial’s final
results. To ensure the integrity of the
trial and the validity of its findings, the
DMC guidance strongly recommends
maintaining the confidentiality of
interim data until the trial completion.
E. Partial Disclosure of Interim Trial
Results by FDA and the Purpose of This
Hearing
Once FDA sends an approval letter for
a new drug, the FD&C Act and FDA
regulations require that a summary or
summaries of the safety and
effectiveness data and information
submitted with or incorporated by
reference in the application be made
available immediately for public
disclosure, with certain limited
redactions. FDA’s analyses of the safety
and effectiveness data and information
from clinical studies that support the
approval of a new drug are typically
disclosed with little or no redaction.
However, data relied on to make
approval decisions are ordinarily
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derived from fully completed clinical
trials. In the case of T2DM therapies
where a single, large CVOT to rule out
CV risk was designed to meet both the
requirement for approval and the
postmarketing requirements, approval
would indicate that the study had
indeed ruled out the risk ratio of 1.8, so
this aspect of the interim results would
be known. But that fact would not
reveal the detailed result, e.g., a finding
that CV events were actually reduced by
the drug in the interim analysis.
Disclosure of detailed and more
extensive information or analyses from
an ongoing trial, that is, the results of an
interim analysis, could undermine the
integrity of the trial and jeopardize its
continuation, which could delay or even
prevent obtaining the safety data about
serious risks that were required to be
assessed at the time of approval.
For example, in connection with a
recent approval decision of a drug to
treat T2DM (see MEMORANDA:
Disclosure of Interim Cardiovascular
Risk Study Data, NDA 22271, Nesina
(alogliptin) tablets, and Its Fixed-Dose
Combination Product NDAs 22426 and
203414, dated March 12, 2013, and
Disclosure of Interim Cardiovascular
Risk Study Data and Information Relied
on to Approve, NDA 22271, Nesina
(alogliptin) tablets, and Its Fixed-Dose
Combination Product NDAs 22426 and
203414, dated March 12, 2013, available
at https://www.fda.gov/Drugs/News
Events/ucm398454.htm), FDA released
information at the time of approval that
was considered not likely to undermine
the integrity of the ongoing trial,
including (1) general background and
study information; (2) high-level
summary conclusions that the trial
ruled out the prespecified risk margin
recommended by FDA guidance; and (3)
other data and information from the trial
unrelated to CV risk. FDA decided,
however, to delay disclosure of other
information that it determined could
jeopardize successful completion of the
trial, specifically point estimates of
hazard ratios and associated confidence
intervals for CV risk and detailed data
on CV events and rates. Based on the
circumstances of this case, FDA
determined that delaying disclosure of
these data was appropriate for a limited
time. This information would become
available when FDA completed its
review of the final CV risk study report
and had taken any related regulatory
action based on the final results.
The Agency is holding this hearing to
solicit input from stakeholders on the
effects of disclosing information or
analyses, at various levels of detail, from
an ongoing trial, and whether general
information about the trial can be
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disclosed without significant risk to the
integrity of the trial or its completion.
Making a determination about the effect
of disclosure on a particular trial
requires consideration of the details of
that trial and relevant context.
II. Scope of Public Input Requested
FDA is seeking input from the various
stakeholders on the following issues:
• When a trial to evaluate CV safety of
a new treatment is ongoing at the
time a drug is approved, do
stakeholders agree that disclosure of
detailed analyses (such as point
estimates of hazard ratios and the
associated confidence intervals)
could undermine the integrity of an
ongoing trial and jeopardize its
continuation, potentially
eliminating or substantially
delaying the Agency’s ability to
obtain needed long-term safety
information?
Æ What interim findings, if disclosed,
would represent the greatest risk to
trial integrity or jeopardize trial
continuation?
Æ Can partial disclosure of interim
findings at the time of approval,
essentially disclosing only that the
standard for approval has been met,
offer protection of trial integrity and
also provide health care
practitioners with the essential
scientific information needed to
inform their use of the drug?
Æ If the detailed interim results were
disclosed at the time of approval,
and the ongoing study was
discontinued at that time, would it
be feasible to conduct a new large
trial as a postmarketing requirement
that would fulfill the original study
objective?
• Are there other, alternative trial
designs that would allow for
disclosure of interim results on
safety risks at the time of product
approval while also allowing for
further information to be obtained
postmarket?
III. Notice of Hearing Under 21 CFR
Part 15
The Commissioner of Food and Drugs
is announcing that the public hearing
will be held in accordance with part 15
(21 CFR part 15). The hearing will be
conducted by a presiding officer, who
will be accompanied by FDA senior
management from the Office of the
Commissioner and the Center for Drug
Evaluation and Research.
Under § 15.30(f), the hearing is
informal and the rules of evidence do
not apply. No participant may interrupt
the presentation of another participant.
Only the presiding officer and panel
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41151
members may question any person
during or at the conclusion of each
presentation.
Public hearings under part 15 are
subject to FDA’s policy and procedures
for electronic media coverage of FDA’s
public administrative proceedings (part
10, subpart C (21 CFR part 10, subpart
C)). Under § 10.205, representatives of
the electronic media may be permitted,
subject to certain limitations, to
videotape, film, or otherwise record
FDA’s public administrative
proceedings, including presentations by
participants. The hearing will be
transcribed as stipulated in § 15.30(b)
(see section VI for more details). To the
extent that the conditions for the
hearing, as described in this notice,
conflict with any provisions set out in
part 15, this notice acts as a waiver of
those provisions as specified in
§ 15.30(h).
IV. Attendance and Registration
The FDA Conference Center at the
White Oak location is a Federal facility
with security procedures and limited
seating. Individuals who wish to attend
the public hearing must register on or
before July 28, 2014, by visiting https://
www.surveymonkey.com/s/7L8Z66Q
and contacting Indira Hills (see FOR
FURTHER INFORMATION CONTACT). Early
registration is recommended.
Registration is free and will be on a firstcome, first-served basis. However, FDA
may limit the number of participants
from each organization based on space
limitations. Onsite registration on the
day of the hearing will be based on
space availability.
FDA will provide additional
background information at the time the
Federal Register notice is published and
an agenda approximately 2 weeks before
the hearing at FDA Meeting Information
page, which is available online at https://
www.fda.gov/Drugs/NewsEvents/
ucm398454.htm.
Time will be reserved during the
hearing for planned presentations from
the audience. If you would like to
present at the hearing, please indicate
this in your hearing registration. Time
for audience presentations is limited
and will be assigned on a first-come,
first-served basis. Note also that time
will be designated throughout the day
for general comments and questions
from the audience following the panel
discussions.
In this Federal Register notice, FDA
has included specific issues that will be
addressed by the panel. If you wish to
address one or more of these issues in
your presentation, please indicate this at
the time you register so that FDA can
consider that in organizing the
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presentations. FDA will do its best to
accommodate requests to speak, and
will determine the amount of time
allotted to each presenter and the
approximate time that each oral
presentation is scheduled to begin.
If you need special accommodations
because of disability, please contact
Indira Hills (see FOR FURTHER
INFORMATION CONTACT) at least 7 days
before the hearing.
A live webcast of this hearing will be
viewable at https://
collaboration.fda.gov/dmcidcvtpart15/
on the day of the hearing. A video
record of the hearing will be available
at the same Web address for 1 year.
V. Comments
Regardless of attendance at the public
hearing, interested persons may submit
either electronic comments regarding
this document to https://
www.regulations.gov or written
comments to the Division of Dockets
Management (see ADDRESSES). It is only
necessary to send one set of comments.
Identify comments with the docket
number found in brackets in the
heading of this document. Received
comments may be seen in the Division
of Dockets Management between 9 a.m.
and 4 p.m., Monday through Friday, and
will be posted to the docket at https://
www.regulations.gov.
VI. Transcripts
As soon as a transcript is available, it
will be accessible at https://
www.regulations.gov. It may be viewed
at the Division of Dockets Management
(see ADDRESSES). A transcript will also
be available in either hard copy or on
CD–ROM, after submission of a
Freedom of Information request. Written
requests are to be sent to Division of
Freedom of Information (ELEM–1029),
Food and Drug Administration, 12420
Parklawn Dr., Element Bldg., Rockville,
MD 20857.
Dated: July 8, 2014.
Leslie Kux,
Assistant Commissioner for Policy.
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DEPARTMENT OF THE TREASURY
Internal Revenue Service
26 CFR Part 301
RIN 1545–BL59
[REG–120756–13]
Disclosures of Return Information
Reflected on Returns to Officers and
Employees of the Department of
Commerce for Certain Statistical
Purposes and Related Activities
Internal Revenue Service (IRS),
Treasury.
ACTION: Notice of proposed rulemaking
by cross-reference to temporary
regulation.
AGENCY:
In the Rules and Regulations
section of this Federal Register the IRS
is issuing temporary regulations
authorizing the disclosure of specified
return information to the Bureau of the
Census (Bureau) for the design of a
decennial census that costs less per
housing unit and still maintains high
quality results. The temporary
regulations are made pursuant to a
request from the Secretary of Commerce.
These regulations require no action by
taxpayers and have no effect on their tax
liabilities. Thus, no taxpayers are likely
to be affected by the disclosures
authorized by this guidance. The text of
the temporary regulations published in
the Rules and Regulations section of the
Federal Register serves as the text of
these proposed regulations.
DATES: Written and electronic comments
and requests for a public hearing must
be received by October 14, 2014.
ADDRESSES: Send submissions to:
CC:PA:LPD:PR (REG–120756–13), Room
5203, Internal Revenue Service, Post
Office Box 7604, Ben Franklin Station,
Washington, DC 20044. Submissions
may be hand-delivered Monday through
Friday between the hours of 8 a.m. and
4 p.m. to CC:PA:LPD:PR (REG–120756–
13), Courier’s Desk, Internal Revenue
Service, 1111 Constitution Avenue NW.,
Washington, DC 20224, or sent
electronically, via the Federal
eRulemaking Portal at
www.regulations.gov (IRS REG–120756–
13).
FOR FURTHER INFORMATION CONTACT:
Concerning the proposed regulations,
Melissa Avrutine, (202) 317–6833;
concerning submissions of comments,
Oluwafunmilayo Taylor, (202) 317–5179
(not toll-free numbers).
SUPPLEMENTARY INFORMATION:
SUMMARY:
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Background
This document contains proposed
amendments to 26 CFR Part 301 relating
to section 6103(j)(1)(A) of the Internal
Revenue Code (Code). Section
6103(j)(1)(A) authorizes the Secretary of
the Treasury to furnish, upon written
request by the Secretary of Commerce,
such return or return information as the
Secretary of Treasury may prescribe by
regulation to officers and employees of
the Bureau for the purpose of, but only
to the extent necessary in, the
structuring of censuses and conducting
related statistical activities authorized
by law. Section 301.6103(j)(1)–1 of the
regulations further defines such
purposes by reference to 13 U.S.C.
chapter 5 and provides an itemized
description of the return information
authorized to be disclosed for such
purposes. This document contains
proposed regulations authorizing the
disclosure of additional items of return
information requested by the Secretary
of Commerce. Temporary regulations in
the Rules and Regulations section of this
issue of the Federal Register amend 26
CFR part 301. The text of those
temporary regulations serves as the text
of these proposed regulations. The
preamble to the temporary regulations
explains the temporary regulations and
these proposed regulations.
Special Analyses
It has been determined that this notice
of proposed rulemaking is not a
significant regulatory action as defined
in Executive Order 12866, as
supplemented by Executive Order
13563. Therefore, a regulatory
assessment is not required. It also has
been determined that section 553(b) of
the Administrative Procedures Act (5
U.S.C. chapter 5) does not apply to these
regulations, and because the regulation
does not impose a collection of
information on small entities, the
Regulatory Flexibility Act (5 U.S.C.
chapter 6) does not apply. Pursuant to
section 7805(f) of the Code, this
regulation has been submitted to the
Chief Counsel for Advocacy of the Small
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on its impact on small business.
Comments and Requests for Public
Hearing
Before these proposed regulations are
adopted as final regulations,
consideration will be given to any
comments that are submitted timely to
the IRS as prescribed in this preamble
under the ADDRESSES heading. The IRS
and Treasury Department request
comments on all aspects of the proposed
regulations. All comments that are
E:\FR\FM\15JYP1.SGM
15JYP1
]]>Agencies
[Federal Register Volume 79, Number 135 (Tuesday, July 15, 2014)]
[Proposed Rules]
[Pages 41149-41152]
From the Federal Register Online via the Government Printing Office [www.gpo.gov]
[FR Doc No: 2014-16374]
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DEPARTMENT OF HEALTH AND HUMAN SERVICES
Food and Drug Administration
21 CFR Part 15
[Docket No. FDA-2014-N-0824]
Confidentiality of Interim Results in Cardiovascular Outcome
Safety Trials; Public Hearing; Request for Comments
AGENCY: Food and Drug Administration, HHS.
ACTION: Notification of public hearing; request for comments.
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SUMMARY: The Food and Drug Administration (FDA) is announcing a public
hearing that will provide a forum to discuss confidentiality of interim
results for certain cardiovascular outcomes trials (CVOTs) submitted to
the Agency while the trials are still ongoing. The purpose of the
public hearing is to initiate constructive discussion among regulators,
researchers, health care providers, representatives from the
pharmaceutical industry and health care organizations, and the general
public, about appropriate handling of interim analysis results of these
ongoing CVOTs. FDA is also opening a public docket to receive comments
on this topic.
DATES: The public hearing will be held on August 11, 2014, from 8 a.m.
to 5 p.m. Individuals who wish to present at the public hearing must
register by July 28, 2014. Section IV provides attendance and
registration information. To ensure consideration, submit comments by
July 28, 2014. Electronic or written comments will be accepted after
the public hearing until October 10, 2014.
ADDRESSES: The public hearing will be held at the FDA White Oak Campus,
10903 New Hampshire Ave., Bldg. 31 Conference Center, the Great Room
(rm. 1503), Silver Spring, MD 20993-0002. Entrance for the public
hearing participants (non-FDA employees) is through Building 1 where
routine security check procedures will be performed. For parking and
security information, please refer to https://www.fda.gov/AboutFDA/WorkingatFDA/BuildingsandFacilities/WhiteOakCampusInformation/ucm241740.htm.
Submit electronic comments to https://www.regulations.gov. Submit
written comments to the Division of Dockets Management (HFA-305), Food
and Drug Administration, 5630 Fishers Lane, rm. 1061, Rockville, MD
20852. Identify comments with the docket number found in brackets in
the heading of this document.
FOR FURTHER INFORMATION CONTACT: Indira Hills, Food and Drug
Administration, Center for Drug Evaluation and Research, 10903 New
Hampshire Ave., Bldg. 21, rm. 4508, Silver Spring, MD 20993, 301-796-
9686, FAX: 301-796-9907, email: indira.hills@fda.hhs.gov.
SUPPLEMENTARY INFORMATION:
I. Background
A. The Requirement for Postmarketing Studies To Assess the Risk of a
New Drug
In some cases, studies submitted to FDA as part of a new drug
application or biologics license application will demonstrate that a
drug is safe and effective for its intended use (i.e., that its
benefits outweigh its identified risks), but the Agency will
nevertheless require a sponsor to conduct additional postmarketing
studies or trials under section 505(o)(3) of the Federal Food, Drug,
and Cosmetic Act (the FD&C Act)
[[Page 41150]]
(21 U.S.C. 355(o)(3)) for the following reasons: To assess a known
serious risk related to use of the drug, to assess signals of a serious
risk related to use of the drug, or to identify an unexpected risk when
available data indicate the potential for a serious risk.
B. FDA's Approach to the Approval of Drugs To Treat Type II Diabetes
For most drugs, clinical trials of reasonable size can establish a
favorable relationship of benefit to relatively common risks, but they
are not large enough to assess the risk of rare serious events such as
heart attacks, strokes, or death. Where there is concern about these
risks (e.g., concern about drugs to treat Type II diabetes mellitus
(T2DM) or to promote weight loss), development programs include CVOTs
to help assess the risk to meet the requirements for drug approval. In
some cases, applicants have conducted a metaanalysis of cardiovascular
(CV) risk from Phase 2/3 trials to help establish the safety of a drug
and a separate larger CVOT as a postmarketing requirement under section
505(o)(3) of the FD&C Act. In other cases, analyses of interim data
from a single CVOT will demonstrate that a drug is safe with regard to
CV risk for its intended use, and, if the overall risk-benefit analysis
supports approval, the applicant will further assess the CV risks by
continuing the trial as a postmarketing requirement.
The Agency has described its expectations for CV outcome data for
drugs to treat T2DM in the guidance for industry ``Diabetes Mellitus
Evaluating Cardiovascular Risk in New Antidiabetic Therapies to Treat
Type 2'' (available at Diabetes'' (https://www.fda.gov/downloads/Drugs/GuidanceComplianceRegulatoryInformation/Guidances/UCM071627.pdf), which
was issued based on the discussion at an advisory committee meeting,\1\
as well as in other available data and information. The guidance makes
recommendations about how to demonstrate that a new therapy to treat
T2DM is not associated with an unacceptable increase in CV risk.
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\1\ On July 1 and 2, 2008, the Endocrinologic and Metabolic Drug
Advisory Committee met to discuss the role of CV assessment in the
premarketing and postmarketing settings (https://www.fda.gov/ohrms/dockets/ac/cder08.html#endocrinologicmetabolic).
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The guidance states that before submission of a new drug
application (NDA) or biologics license application, the premarketing CV
outcome data should show that the incidence of important CV events
occurring with the investigational agent is not more than 80 percent
increase compared to the control group (i.e., that the upper bound of
the 2-sided 95 percent confidence interval for the estimated risk ratio
for CV events is less than 1.8). The guidance also states that if the
risk ratio is between 1.3 and 1.8 and the overall risk-benefit analysis
supports approval, a postmarketing trial will generally be necessary to
show that the upper bound of the 2-sided 95 percent confidence interval
for the estimated risk ratio is less than 1.3. This showing can be
achieved by conducting an adequately powered new postmarketing trial,
by combining results of separate premarketing and postmarketing trials,
or by continuing a large CVOT in which a planned interim analysis is
the basis for concluding that the risk ratio is less than 1.8. If the
risk ratio of 1.3 is ruled out based on premarket data, then a
postmarketing requirement may not be necessary.
C. Interim Analyses, the Importance of Their Confidentiality, and the
Role of the Data Monitoring Committee
Interim analyses are analyses of study data conducted partway
through an ongoing clinical trial. They can play an integral role in
clinical trials by allowing for the safety of enrolled patients to be
monitored at various intervals in the study and also by allowing for
the possibility of stopping the trial early for safety concerns, for
futility, or for early evidence of efficacy that would make it
unethical for the trial to proceed. Confidentiality of interim data is
a paramount concern: The 1998 International Conference on Harmonization
(ICH) guidance for industry ``E9 Statistical Principles for Clinical
Trials'' (ICH E9 guidance) (available at https://www.fda.gov/downloads/Drugs/GuidanceComplianceRegulatoryInformation/Guidances/ucm073137.pdf)
reflects a collective view across regulatory agencies in the European
Union, Japan, and the United States when it states that ``All staff
involved in the conduct of the trial should remain blind to the results
of such analyses, because of the possibility that their attitudes to
the trial will be modified and cause changes in the characteristics of
patients to be recruited or biases in treatment comparisons.''
An independent Data Monitoring Committee (DMC) is usually
established to review the interim analysis results and make
recommendations to the sponsor about any action needed based on those
results, allowing the sponsor and other personnel associated with the
trial to remain masked to interim results. In 2006, FDA issued the
guidance for clinical trial sponsors ``Establishment and Operation of
Clinical Trial Data Monitoring Committees'' (DMC guidance) (available
at https://www.fda.gov/downloads/RegulatoryInformation/Guidances/UCM127073.pdf) that reiterated many of the best practices for interim
analyses and DMCs outlined in the ICH E9 guidance. Specifically, the
guidance states that ``[p]rocedures should be established to safeguard
confidential interim data from the project team, investigators, sponsor
representatives, or anyone else outside the DMC and the statistician(s)
performing the interim analyses (see 21 CFR 314.126(b)(5) (drugs) and
21 CFR 860.7(f)(1) (devices)).'' An exception is made in considering
the need to disseminate safety data to allow for appropriate monitoring
of patients' safety.
D. Potential Adverse Consequences of Disclosure of Interim Results
The concern with widespread disclosure of interim results in an
ongoing trial, as described in the DMC guidance, stems from the
potential of the disclosure to negatively affect the conduct of the
remaining portion of the trial. The impact could include unanticipated
changes in recruitment, treatment administration, or other aspects of
trial conduct, as well as loss of objectivity in safety event
reporting. Sponsors and other interested parties with access to interim
data may have difficulty managing the remainder of the trial in an
objective manner, particularly if changes to the trial protocol are
needed for other reasons. Knowledge of interim data may influence
decisions about the trial going forward, and it is nearly impossible to
assess the impact of that influence on the trial's final results. To
ensure the integrity of the trial and the validity of its findings, the
DMC guidance strongly recommends maintaining the confidentiality of
interim data until the trial completion.
E. Partial Disclosure of Interim Trial Results by FDA and the Purpose
of This Hearing
Once FDA sends an approval letter for a new drug, the FD&C Act and
FDA regulations require that a summary or summaries of the safety and
effectiveness data and information submitted with or incorporated by
reference in the application be made available immediately for public
disclosure, with certain limited redactions. FDA's analyses of the
safety and effectiveness data and information from clinical studies
that support the approval of a new drug are typically disclosed with
little or no redaction. However, data relied on to make approval
decisions are ordinarily
[[Page 41151]]
derived from fully completed clinical trials. In the case of T2DM
therapies where a single, large CVOT to rule out CV risk was designed
to meet both the requirement for approval and the postmarketing
requirements, approval would indicate that the study had indeed ruled
out the risk ratio of 1.8, so this aspect of the interim results would
be known. But that fact would not reveal the detailed result, e.g., a
finding that CV events were actually reduced by the drug in the interim
analysis. Disclosure of detailed and more extensive information or
analyses from an ongoing trial, that is, the results of an interim
analysis, could undermine the integrity of the trial and jeopardize its
continuation, which could delay or even prevent obtaining the safety
data about serious risks that were required to be assessed at the time
of approval.
For example, in connection with a recent approval decision of a
drug to treat T2DM (see MEMORANDA: Disclosure of Interim Cardiovascular
Risk Study Data, NDA 22271, Nesina (alogliptin) tablets, and Its Fixed-
Dose Combination Product NDAs 22426 and 203414, dated March 12, 2013,
and Disclosure of Interim Cardiovascular Risk Study Data and
Information Relied on to Approve, NDA 22271, Nesina (alogliptin)
tablets, and Its Fixed-Dose Combination Product NDAs 22426 and 203414,
dated March 12, 2013, available at https://www.fda.gov/Drugs/NewsEvents/ucm398454.htm), FDA released information at the time of approval that
was considered not likely to undermine the integrity of the ongoing
trial, including (1) general background and study information; (2)
high-level summary conclusions that the trial ruled out the
prespecified risk margin recommended by FDA guidance; and (3) other
data and information from the trial unrelated to CV risk. FDA decided,
however, to delay disclosure of other information that it determined
could jeopardize successful completion of the trial, specifically point
estimates of hazard ratios and associated confidence intervals for CV
risk and detailed data on CV events and rates. Based on the
circumstances of this case, FDA determined that delaying disclosure of
these data was appropriate for a limited time. This information would
become available when FDA completed its review of the final CV risk
study report and had taken any related regulatory action based on the
final results.
The Agency is holding this hearing to solicit input from
stakeholders on the effects of disclosing information or analyses, at
various levels of detail, from an ongoing trial, and whether general
information about the trial can be disclosed without significant risk
to the integrity of the trial or its completion. Making a determination
about the effect of disclosure on a particular trial requires
consideration of the details of that trial and relevant context.
II. Scope of Public Input Requested
FDA is seeking input from the various stakeholders on the following
issues:
When a trial to evaluate CV safety of a new treatment is
ongoing at the time a drug is approved, do stakeholders agree that
disclosure of detailed analyses (such as point estimates of hazard
ratios and the associated confidence intervals) could undermine the
integrity of an ongoing trial and jeopardize its continuation,
potentially eliminating or substantially delaying the Agency's ability
to obtain needed long-term safety information?
[cir] What interim findings, if disclosed, would represent the
greatest risk to trial integrity or jeopardize trial continuation?
[cir] Can partial disclosure of interim findings at the time of
approval, essentially disclosing only that the standard for approval
has been met, offer protection of trial integrity and also provide
health care practitioners with the essential scientific information
needed to inform their use of the drug?
[cir] If the detailed interim results were disclosed at the time of
approval, and the ongoing study was discontinued at that time, would it
be feasible to conduct a new large trial as a postmarketing requirement
that would fulfill the original study objective?
Are there other, alternative trial designs that would allow
for disclosure of interim results on safety risks at the time of
product approval while also allowing for further information to be
obtained postmarket?
III. Notice of Hearing Under 21 CFR Part 15
The Commissioner of Food and Drugs is announcing that the public
hearing will be held in accordance with part 15 (21 CFR part 15). The
hearing will be conducted by a presiding officer, who will be
accompanied by FDA senior management from the Office of the
Commissioner and the Center for Drug Evaluation and Research.
Under Sec. 15.30(f), the hearing is informal and the rules of
evidence do not apply. No participant may interrupt the presentation of
another participant. Only the presiding officer and panel members may
question any person during or at the conclusion of each presentation.
Public hearings under part 15 are subject to FDA's policy and
procedures for electronic media coverage of FDA's public administrative
proceedings (part 10, subpart C (21 CFR part 10, subpart C)). Under
Sec. 10.205, representatives of the electronic media may be permitted,
subject to certain limitations, to videotape, film, or otherwise record
FDA's public administrative proceedings, including presentations by
participants. The hearing will be transcribed as stipulated in Sec.
15.30(b) (see section VI for more details). To the extent that the
conditions for the hearing, as described in this notice, conflict with
any provisions set out in part 15, this notice acts as a waiver of
those provisions as specified in Sec. 15.30(h).
IV. Attendance and Registration
The FDA Conference Center at the White Oak location is a Federal
facility with security procedures and limited seating. Individuals who
wish to attend the public hearing must register on or before July 28,
2014, by visiting https://www.surveymonkey.com/s/7L8Z66Q and contacting
Indira Hills (see FOR FURTHER INFORMATION CONTACT). Early registration
is recommended. Registration is free and will be on a first-come,
first-served basis. However, FDA may limit the number of participants
from each organization based on space limitations. Onsite registration
on the day of the hearing will be based on space availability.
FDA will provide additional background information at the time the
Federal Register notice is published and an agenda approximately 2
weeks before the hearing at FDA Meeting Information page, which is
available online at https://www.fda.gov/Drugs/NewsEvents/ucm398454.htm.
Time will be reserved during the hearing for planned presentations
from the audience. If you would like to present at the hearing, please
indicate this in your hearing registration. Time for audience
presentations is limited and will be assigned on a first-come, first-
served basis. Note also that time will be designated throughout the day
for general comments and questions from the audience following the
panel discussions.
In this Federal Register notice, FDA has included specific issues
that will be addressed by the panel. If you wish to address one or more
of these issues in your presentation, please indicate this at the time
you register so that FDA can consider that in organizing the
[[Page 41152]]
presentations. FDA will do its best to accommodate requests to speak,
and will determine the amount of time allotted to each presenter and
the approximate time that each oral presentation is scheduled to begin.
If you need special accommodations because of disability, please
contact Indira Hills (see FOR FURTHER INFORMATION CONTACT) at least 7
days before the hearing.
A live webcast of this hearing will be viewable at https://collaboration.fda.gov/dmcidcvtpart15/ on the day of the hearing. A
video record of the hearing will be available at the same Web address
for 1 year.
V. Comments
Regardless of attendance at the public hearing, interested persons
may submit either electronic comments regarding this document to https://www.regulations.gov or written comments to the Division of Dockets
Management (see ADDRESSES). It is only necessary to send one set of
comments. Identify comments with the docket number found in brackets in
the heading of this document. Received comments may be seen in the
Division of Dockets Management between 9 a.m. and 4 p.m., Monday
through Friday, and will be posted to the docket at https://www.regulations.gov.
VI. Transcripts
As soon as a transcript is available, it will be accessible at
https://www.regulations.gov. It may be viewed at the Division of Dockets
Management (see ADDRESSES). A transcript will also be available in
either hard copy or on CD-ROM, after submission of a Freedom of
Information request. Written requests are to be sent to Division of
Freedom of Information (ELEM-1029), Food and Drug Administration, 12420
Parklawn Dr., Element Bldg., Rockville, MD 20857.
Dated: July 8, 2014.
Leslie Kux,
Assistant Commissioner for Policy.
[FR Doc. 2014-16374 Filed 7-14-14; 8:45 am]
BILLING CODE 4164-01-P
