Public Workshop on Minimal Residual Disease; Public Workshop, 76051-76052 [2012-31044]
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Federal Register / Vol. 77, No. 247 / Wednesday, December 26, 2012 / Notices
The public workshop will be
held on March 4, 2013, from 8 a.m. to
4 p.m.
ADDRESSES: The public workshop will
be held at the FDA White Oak Campus,
10903 New Hampshire Ave., Building
31 Conference Center, the Great Room
(rm. 1503), Silver Spring, MD 20993–
0002. Entrance for the public workshop
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.
FOR FURTHER INFORMATION CONTACT:
Christine Lincoln, Center for Drug
Evaluation and Research, Food and
Drug Administration, 10903 New
Hampshire Ave., Bldg. 22, rm. 6413,
Silver Spring, MD 20993–0002, 301–
796–2340, email:
Christine.Lincoln@fda.hhs.gov.
SUPPLEMENTARY INFORMATION:
tkelley on DSK3SPTVN1PROD with
DATES:
I. Background
Complete remission, relapse-free
survival, and overall survival are
frequently used as endpoints in clinical
trials of new therapeutics for AML.
These endpoints have some limitations,
especially in the context of minimal
residual disease. Use of morphological
complete remission may miss
individuals with clinically significant
residual disease who are not truly in
remission. For those being followed
after remission induction, new evidence
of submorphological disease may
prompt therapy before morphological
relapse. Additionally, for patients with
good prognosis, the length of the
clinical trial followup may be very long
when survival is the outcome measured,
raising logistical and financial
challenges for study conduct. More
information is needed on whether MRD
in AML can be qualified as a response
biomarker and then used as a clinical
trial endpoint and what the challenges
would be to implement use of such an
endpoint.
This Public Workshop on Minimal
Residual Disease in AML will be one of
a series of FDA workshops to establish
processes and procedures necessary to
qualify a prognostic biomarker, MRD, as
a possible response or efficacy
biomarker in a group of hematological
malignancies. Evaluation of clinical data
suggests that MRD can be established as
a potential surrogate endpoint for
pivotal clinical trials and drug approval
given its prominent role as a prognostic
indicator in certain subtypes of acute
and chronic leukemia. The Office of
VerDate Mar<15>2010
06:31 Dec 22, 2012
Jkt 229001
Hematology and Oncology Products has
explored, or plans to explore, the
potential utility of MRD as a surrogate
endpoint in acute lymphoblastic
leukemia (ALL) (including the relapsed
setting), chronic lymphocytic leukemia
(CLL), and AML. Given the diverse
pathophysiology and natural history of
these diseases and current practice
standards, individualized consideration
of MRD as a surrogate endpoint is
warranted. The ALL workshop was held
on April 18, 2012, and the CLL
workshop will be held on February 27,
2013.
II. Structure and Scope of the
Workshop
The workshop’s scope will include
discussions of the use of flow cytometry
and molecular methods used to detect
and measure minimal residual disease
in patients being treated for AML. The
workshop will consist of formal
presentations examining the regulatory,
scientific, and clinical basis for use of
biomarkers as potential clinical trial
endpoints in AML interspersed with
discussions on issues associated with
these endpoints.
III. Attendance and Registration
FDA encourages patient advocates,
representatives from industry, consumer
groups, health care professionals,
researchers, and other interested
persons to attend this public workshop.
There is no registration fee for the
public workshop. To register
electronically, please use the following
Web site: https://www.zoomerang.com/
Survey/WEB22GPAXN9NQB (FDA has
verified the Web site address, but we are
not responsible for any subsequent
changes to the Web site after this
document publishes in the Federal
Register.) Seats are limited and
conference space will be filled in the
order in which registrations are
received. Onsite registration will be
available to the extent that space is
available on the day of the conference.
Information regarding special
accommodations due to a disability,
visitor parking, and transportation may
be accessed at: https://www.fda.gov/
AdvisoryCommittees/default.htm.
Under the heading ‘‘Resources for You,’’
click on ‘‘Public Meetings at the FDA
White Oak Campus.’’
Dated: December 20, 2012.
Leslie Kux,
Assistant Commissioner for Policy.
[FR Doc. 2012–31043 Filed 12–21–12; 4:15 pm]
BILLING CODE 4160–01–P
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76051
DEPARTMENT OF HEALTH AND
HUMAN SERVICES
Food and Drug Administration
[Docket No. FDA–2012–N–0001]
Public Workshop on Minimal Residual
Disease; Public Workshop
AGENCY:
Food and Drug Administration,
HHS.
ACTION:
Notice of public workshop.
The Food and Drug
Administration (FDA), in cosponsorship
with the American Society of Clinical
Oncology, is announcing a public
workshop that will provide a forum for
discussion of extending the
qualification of minimal residual
disease (MRD) detection as a prognostic
biomarker to that of an efficacy/
response biomarker in evaluating new
drugs for the treatment of chronic
lymphocytic leukemia (CLL). Our
objective for the workshop is to provide
a venue for an in-depth discussion of
potential surrogate endpoints for trials
intended to support the approval of new
drugs or biologics for the treatment of
CLL. Participants in the workshop will
examine the advantages and
disadvantages of MRD as a surrogate
endpoint for approval, identify the
preferred technology platform and
performance characteristics for the assay
of this biomarker, and discuss any
issues regarding methodological
standardization for the biomarker. The
primary focus will be on the biomarkers
that are ready for incorporation into
clinical trials and the technical and
regulatory challenges for use of these
markers.
SUMMARY:
The public workshop will be
held on February 27, 2013, from 8 a.m.
to 4 p.m.
ADDRESSES: The public workshop will
be held at the FDA White Oak Campus,
10903 New Hampshire Ave., Building
31 Conference Center, the Great Room
(rm. 1503), Silver Spring, MD 20993–
0002. Entrance for the public workshop
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.
FOR FURTHER INFORMATION CONTACT:
Christine Lincoln, Center for Drug
Evaluation and Research, Food and
Drug Administration, 10903 New
Hampshire Ave., Bldg. 22, rm. 6413,
Silver Spring, MD 20993–0002, 301–
DATES:
E:\FR\FM\26DEN1.SGM
26DEN1
76052
Federal Register / Vol. 77, No. 247 / Wednesday, December 26, 2012 / Notices
796–2340, email: Christine.Lincoln@fda.
hhs.gov.
SUPPLEMENTARY INFORMATION:
I. Background
The Public Workshop on Minimal
Residual Disease will be one of a series
of FDA workshops to establish
processes and procedures necessary to
qualify a prognostic biomarker, MRD, as
a possible response or efficacy
biomarker in a group of hematological
malignancies. Evaluation of clinical data
suggests that MRD can be established as
a potential surrogate endpoint for
pivotal clinical trials and drug approval
given its prominent role as a prognostic
indicator in certain subtypes of acute
and chronic leukemia. The Office of
Hematology and Oncology Products
plans to explore the potential utility of
MRD as a surrogate endpoint in acute
lymphoblastic leukemia (ALL)
(including the relapsed setting), CLL,
and acute myeloid leukemia (AML).
Given the diverse pathophysiology and
natural history of these diseases, and
current practice standards,
individualized consideration of MRD as
a surrogate endpoint is warranted. The
ALL workshop was held on April 18,
2012. The CLL and AML workshops are
scheduled for February 27, 2013, and
March 4, 2013, respectively.
tkelley on DSK3SPTVN1PROD with
II. Structure and Scope of the
Workshop
The workshop’s scope will extend to
the use of flow cytometry and the
molecular methods used to measure
minimal residual disease in patients
being treated for CLL. The workshop
will consist of formal presentations
examining the regulatory, scientific, and
clinical basis for use of biomarkers as
potential clinical trial endpoints in CLL
followed by discussions on issues
associated with use of an MRD
endpoint.
III. Attendance and Registration
FDA encourages patient advocates,
representatives from industry, consumer
groups, health care professionals,
researchers, and other interested
persons to attend this public workshop.
There is no registration fee for the
public workshop. To register
electronically, please use the following
Web site: https://www.zoomerang.com/
Survey/WEB22GPA3U95QX (FDA has
verified the Web site address, but we are
not responsible for any subsequent
changes to the Web site after this
document publishes in the Federal
Register.) Seats are limited and
conference space will be filled in the
order in which registrations are
received. Onsite registration will be
VerDate Mar<15>2010
06:31 Dec 22, 2012
Jkt 229001
available to the extent that space is
available on the day of the conference.
Information regarding special
accommodations due to a disability,
visitor parking, and transportation may
be accessed at: https://www.fda.gov/
AdvisoryCommittees/default.htm.
Under the heading ‘‘Resources for You,’’
click on ‘‘Public Meetings at the FDA
White Oak Campus.’’
Dated: December 20, 2012.
Leslie Kux,
Assistant Commissioner for Policy.
[FR Doc. 2012–31044 Filed 12–21–12; 4:15 pm]
BILLING CODE 4160–01–P
DEPARTMENT OF HEALTH AND
HUMAN SERVICES
Health Resources and Services
Administration
Agency Information Collection
Activities: Proposed Collection:
Comment Request
ACTION:
Notice.
In compliance with the
requirement for opportunity for public
comment on proposed data collection
projects (section 3506(c)(2)(A) of Title
44, United States Code, as amended by
the Paperwork Reduction Act of 1995,
Public Law 104–13), the Health
Resources and Services Administration
(HRSA) publishes periodic summaries
of proposed projects being developed
for submission to the Office of
Management and Budget (OMB) under
the Paperwork Reduction Act of 1995.
To request more information on the
proposed project or to obtain a copy of
the data collection plans and draft
instruments, email paperwork@hrsa.gov
or call the HRSA Reports Clearance
Officer at (301) 443–1984.
HRSA especially requests comments
on: (1) The necessity and utility of the
proposed information collection for the
proper performance of the agency’s
function, (2) the accuracy of the
estimated burden, (3) ways to enhance
the quality, utility, and clarity of the
information to be collected, and (4) the
use of automated collection techniques
or other forms of information
technology to minimize the information
collection burden.
SUMMARY:
Information Collection Request Title:
Survey of Eligible Users of the National
Practitioner Data Bank and the
Healthcare Integrity and Protection
Data Bank (OMB No. 0915–xxxx)—New
Abstract: The Health Resources and
Services Administration (HRSA) plans
to conduct a survey of the National
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Practitioner Data Bank and the
Healthcare Integrity and Protection Data
Bank (NPDB/HIPDB). The purpose of
this survey is to assess the overall
satisfaction of the eligible users of the
NPDB/HIPDB. This survey will evaluate
the effectiveness of the NPDB/HIPDB as
flagging systems, sources of information,
and use in decision making.
Furthermore, this survey will collect
information from eligible non-users of
the NPDB/HIPDB to understand what
can be done to aid the eligible non-users
in registering, accessing, and using the
information available in the NPDB/
HIPDB. This survey is a follow-up to the
NPDB/HIPDB users and non-users
survey of 2008.
The survey will be administered to
eligible users of the NPDB/HIPDB. The
survey will also collect information
from those that have had matched
responses. A matched response occurs
when an eligible user queries the NPDB/
HIPDB then receives a report. The
purpose of collecting the matched
response data is to understand what
actions or decisions are made when an
eligible user receives a matched
response.
The survey will be administered to
non-users of the NPDB/HIPDB. Nonusers of the NPDB/HIPDB are
considered eligible users that have (i)
never registered, (ii) registered in the
past but are not currently registered, or
(iii) are registered but are not using the
NPDB/HIPDB. The information
provided by the non-users will enable
understanding of what needs to be done
to facilitate and educate non-users on
accessing and using the information in
the NPDB/HIPDB. Finally, the survey
will be administered to those that use
the self-query service provided by the
NPDB/HIPDB. Understanding self-query
user satisfaction and how the
information is used is an important
component of the survey.
Eligible users of the NPDB/HIPDB
will be asked to complete a web-based
survey. Eligible non-users that have
never registered in the NPDB/HIPDB
will be contacted via telephone to
obtain email information so that they
will be able to complete a web-based
survey. Data gathered from the survey
will be compared with previous survey
results. This survey will provide HRSA
with the information necessary to
improve the usability and effectiveness
of the NPDB/HIPDB.
Burden Statement: Burden in this
context means the time expended by
persons to generate, maintain, retain,
disclose or provide the information
requested. This includes the time
needed to review instructions, to
develop, acquire, install and utilize
E:\FR\FM\26DEN1.SGM
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]]>Agencies
[Federal Register Volume 77, Number 247 (Wednesday, December 26, 2012)]
[Notices]
[Pages 76051-76052]
From the Federal Register Online via the Government Printing Office [www.gpo.gov]
[FR Doc No: 2012-31044]
-----------------------------------------------------------------------
DEPARTMENT OF HEALTH AND HUMAN SERVICES
Food and Drug Administration
[Docket No. FDA-2012-N-0001]
Public Workshop on Minimal Residual Disease; Public Workshop
AGENCY: Food and Drug Administration, HHS.
ACTION: Notice of public workshop.
-----------------------------------------------------------------------
SUMMARY: The Food and Drug Administration (FDA), in cosponsorship with
the American Society of Clinical Oncology, is announcing a public
workshop that will provide a forum for discussion of extending the
qualification of minimal residual disease (MRD) detection as a
prognostic biomarker to that of an efficacy/response biomarker in
evaluating new drugs for the treatment of chronic lymphocytic leukemia
(CLL). Our objective for the workshop is to provide a venue for an in-
depth discussion of potential surrogate endpoints for trials intended
to support the approval of new drugs or biologics for the treatment of
CLL. Participants in the workshop will examine the advantages and
disadvantages of MRD as a surrogate endpoint for approval, identify the
preferred technology platform and performance characteristics for the
assay of this biomarker, and discuss any issues regarding
methodological standardization for the biomarker. The primary focus
will be on the biomarkers that are ready for incorporation into
clinical trials and the technical and regulatory challenges for use of
these markers.
DATES: The public workshop will be held on February 27, 2013, from 8
a.m. to 4 p.m.
ADDRESSES: The public workshop will be held at the FDA White Oak
Campus, 10903 New Hampshire Ave., Building 31 Conference Center, the
Great Room (rm. 1503), Silver Spring, MD 20993-0002. Entrance for the
public workshop 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.
FOR FURTHER INFORMATION CONTACT: Christine Lincoln, Center for Drug
Evaluation and Research, Food and Drug Administration, 10903 New
Hampshire Ave., Bldg. 22, rm. 6413, Silver Spring, MD 20993-0002, 301-
[[Page 76052]]
796-2340, email: Christine.Lincoln@fda.hhs.gov.
SUPPLEMENTARY INFORMATION:
I. Background
The Public Workshop on Minimal Residual Disease will be one of a
series of FDA workshops to establish processes and procedures necessary
to qualify a prognostic biomarker, MRD, as a possible response or
efficacy biomarker in a group of hematological malignancies. Evaluation
of clinical data suggests that MRD can be established as a potential
surrogate endpoint for pivotal clinical trials and drug approval given
its prominent role as a prognostic indicator in certain subtypes of
acute and chronic leukemia. The Office of Hematology and Oncology
Products plans to explore the potential utility of MRD as a surrogate
endpoint in acute lymphoblastic leukemia (ALL) (including the relapsed
setting), CLL, and acute myeloid leukemia (AML). Given the diverse
pathophysiology and natural history of these diseases, and current
practice standards, individualized consideration of MRD as a surrogate
endpoint is warranted. The ALL workshop was held on April 18, 2012. The
CLL and AML workshops are scheduled for February 27, 2013, and March 4,
2013, respectively.
II. Structure and Scope of the Workshop
The workshop's scope will extend to the use of flow cytometry and
the molecular methods used to measure minimal residual disease in
patients being treated for CLL. The workshop will consist of formal
presentations examining the regulatory, scientific, and clinical basis
for use of biomarkers as potential clinical trial endpoints in CLL
followed by discussions on issues associated with use of an MRD
endpoint.
III. Attendance and Registration
FDA encourages patient advocates, representatives from industry,
consumer groups, health care professionals, researchers, and other
interested persons to attend this public workshop. There is no
registration fee for the public workshop. To register electronically,
please use the following Web site: https://www.zoomerang.com/Survey/WEB22GPA3U95QX (FDA has verified the Web site address, but we are not
responsible for any subsequent changes to the Web site after this
document publishes in the Federal Register.) Seats are limited and
conference space will be filled in the order in which registrations are
received. Onsite registration will be available to the extent that
space is available on the day of the conference.
Information regarding special accommodations due to a disability,
visitor parking, and transportation may be accessed at: https://www.fda.gov/AdvisoryCommittees/default.htm. Under the heading
``Resources for You,'' click on ``Public Meetings at the FDA White Oak
Campus.''
Dated: December 20, 2012.
Leslie Kux,
Assistant Commissioner for Policy.
[FR Doc. 2012-31044 Filed 12-21-12; 4:15 pm]
BILLING CODE 4160-01-P
