Request for Information: The National Toxicology Program Interagency Center for the Evaluation of Alternative Toxicological Methods Requests the Nomination of Reference Chemicals, 27323-27324 [2014-10892]
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Federal Register / Vol. 79, No. 92 / Tuesday, May 13, 2014 / Notices
Dated: May 7, 2014.
Carolyn Baum,
Program Analyst, Office of Federal Advisory
Committee Policy.
[FR Doc. 2014–10909 Filed 5–12–14; 8:45 am]
BILLING CODE 4140–01–P
DEPARTMENT OF HEALTH AND
HUMAN SERVICES
National Institutes of Health
Request for Information: The National
Toxicology Program Interagency
Center for the Evaluation of Alternative
Toxicological Methods Requests the
Nomination of Reference Chemicals
The National Toxicology
Program (NTP) Interagency Center for
the Evaluation of Alternative
Toxicological Methods (NICEATM)
requests the nomination of reference
chemicals, with supporting data, to be
used to validate in vitro metabolizing
systems with the potential to interact
with estrogen receptors (ERs) or
androgen receptors (ARs). Specifically, a
list of chemicals is needed to
characterize the usefulness and
limitations of in vitro metabolizing
systems for use in conjunction with ER
and AR transactivation tests.
DATES: The deadline for receipt of
information is June 2, 2014.
ADDRESSES: Nominated reference
chemicals and associated data should be
submitted electronically in Microsoft®
Excel or Word formats to niceatm@
niehs.nih.gov. A Microsoft® Excel
template for data submission is
available at https://ntp.niehs.nih.gov/go/
41493.
FOR FURTHER INFORMATION CONTACT: Dr.
Warren S. Casey, Director, NICEATM;
email: warren.casey@nih.gov; telephone:
(919) 316–4729.
SUPPLEMENTARY INFORMATION:
mstockstill on DSK4VPTVN1PROD with NOTICES
SUMMARY:
Background
Endocrine-active substances (EAS) are
chemicals that interfere with normal
endocrine hormone function by
mimicking, blocking, or increasing their
actions, thereby possibly causing
adverse health effects. United States
legislation (e.g., 7 U.S.C. 136, 110 Stat
1613) requires that chemicals be tested
for their ability to disrupt the hormonal
systems of mammals; prospective
international legislative proposals may
have similar requirements. Chemicals
found to test positive in vitro as EAS
may be in vivo endocrine disruptors.
The lack of in vitro tools that mimic in
vivo metabolism is the main obstacle to
implementation of in vitro tools for EAS
toxicity testing. Improved
VerDate Mar<15>2010
19:27 May 12, 2014
Jkt 232001
understanding of metabolic capabilities
and limitations of in vitro toxicity
testing is critical to:
• Ensure that no potentially active
metabolites are missed
• Allow better interpretation of results
• Accurately predict species-specific
characteristics of absorption,
metabolism, and excretion
While there is a growing body of
international in vitro test guidelines
addressing EAS mechanisms and modes
of action, there are few or no
standardized methods to incorporate
metabolic and toxicokinetic aspects into
these EAS in vitro tests to date. In vitro
assays for EAS should incorporate
metabolic enzyme systems to better
address the relevance of EAS tests to in
vivo adverse outcome pathways.
The Organization for Economic Cooperation and Development (OECD)
Validation Management Group-NonAnimal (VMG–NA) expert working
group develops internationally accepted
non-animal test guidelines to support
various international regulatory needs
for the hazard identification of potential
EAS. These test guidelines describe
methods and approaches capable of
identifying potential EAS without the
use of animals. Consistent with its
purpose of evaluating alternative
methods for testing chemicals and
chemical products, NICEATM
participates in the VMG–NA.
Test guidelines for in vitro assays for
ER activity have been evaluated and
accepted by international regulatory
authorities; test guidelines for in vitro
AR activity assays are currently in
development. However, none of these in
vitro EAS assays account for whole
animal metabolism. Further
development of specific tests is needed
to optimize the use of in vitro
metabolism with EAS assays.
Identification of appropriate reference
chemicals to check the metabolic
capacity of any proposed test method is
key to continued assay development.
For this purpose, the VMG–NA is
developing a robust list of chemicals
that, when metabolized, act as ER or AR
agonist or antagonists.
Request for Information
On behalf of the VMG–NA, NICEATM
requests nominations of chemicals that
can be used to characterize and validate
in vitro metabolizing systems for use in
conjunction with in vitro tests for ER
and AR transactivation. Responses are
requested from all interested parties,
including the research community,
health professionals, educators, policy
makers, industry, and the public.
Considerations for selection of
PO 00000
Frm 00047
Fmt 4703
Sfmt 4703
27323
appropriate chemicals include the
ability of a chemical to act as an ER or
AR agonist or antagonist and:
• Potential for metabolism to make a
chemical either more potent
(bioactivation) or less potent
(detoxification)
• Likelihood of metabolism occurring in
relevant routes of exposure and target
organs
• Likelihood of metabolism occurring
over a range of doses: Information on
the ratio of the half maximal effective
or inhibitory concentration (EC50 or
IC50, respectively) of parent to
daughter metabolites will be useful
and there is a particular need for
information pertaining to substances
where biotransformation yields a very
small or very large ratio of EC50/IC50
of parent to daughter metabolites
• Stability, preferably with real-time
curves and consequent exposure
significance of likely metabolites
• Diversity of likely and predominant
biotransformative pathways
• Diversity of chemical types, use
classes, and consequent applicability
domains
The reference chemicals will be used
to check the metabolic capacity of the in
vitro model, including characterization
of the general metabolic capacity of the
cell lines. To ensure relevant use in a
regulatory context, it will be necessary,
where possible, to make correlations to:
(a) Relevant in vivo metabolic
modeling (accounting for absorption,
distribution, metabolism, and excretion,
etc.) of plasma/blood metabolites in
vertebrate animals (e.g., rat, fish,
human).
(b) Data from the uterotrophic,
Hershberger, and/or other relevant
assays with a demonstrated high
confidence in prediction of
bioactivation of estrogenic or
androgenic agonist and antagonist
pathways, such that the true systemic in
vivo metabolic response is addressed as
accurately as possible.
When reporting the in vitro dose
response for potential reference
chemicals, the concentrations of solvent
and/or carrier proteins used in the assay
buffers to solubilize the reference
chemicals should be described to
facilitate an understanding of potential
differences among new in vitro assays
with regard to free concentrations of
parent chemical and metabolites versus
nominal dosages within each testing
system.
Nominated reference chemicals and
associated data should be submitted
electronically in Microsoft® Excel or
Word formats to niceatm@niehs.nih.gov.
Data submitted can include, but need
E:\FR\FM\13MYN1.SGM
13MYN1
27324
Federal Register / Vol. 79, No. 92 / Tuesday, May 13, 2014 / Notices
not be limited to, citations of reports in
the published literature, data from past
or ongoing validation studies, data in
databases, or unpublished data. A
template for data submission is
available at https://ntp.niehs.nih.gov/go/
41493.
Responses to this request are
voluntary. NICEATM does not intend to
publish a summary of responses
received or any other information
provided. No proprietary, classified,
confidential, or sensitive information
should be included in your response.
Please note that the U.S. Government
will not pay for the preparation of any
information submitted or for its use of
that information.
Those submitting information should
include name, affiliation, mailing
address, phone, fax, email address, and
sponsoring organization (if any) with
the submission. The deadline for receipt
of the requested information is June 2,
2014.
Background Information on NICEATM
NICEATM conducts data analyses,
workshops, independent validation
studies, and other activities to assess
new, revised, and alternative test
methods and strategies and provides
support for the Interagency
Coordinating Committee on the
Validation of Alternative Methods
(ICCVAM). The ICCVAM Authorization
Act of 2000 (42 U.S.C. 285l–3) provides
authority for ICCVAM and NICEATM to
conduct activities relevant to the
development of alternative test
methods. Information about NICEATM
and ICCVAM is found at https://
ntp.niehs.nih.gov/go/niceatm and
https://ntp.niehs.nih.gov/go/iccvam.
Dated: May 7, 2014.
John R. Bucher,
Associate Director, National Toxicology
Program.
[FR Doc. 2014–10892 Filed 5–12–14; 8:45 am]
BILLING CODE 4140–01–P
mstockstill on DSK4VPTVN1PROD with NOTICES
State and county
Alabama:
Jefferson
Docket
1403).
Jefferson
Docket
1403).
Location and case
No.
(FEMA
No.: B–
City of Bessemer
(13–04–7454P).
(FEMA
No.: B–
Unincorporated
areas of Jefferson
County (13–04–
7454P).
VerDate Mar<15>2010
19:27 May 12, 2014
DEPARTMENT OF HOMELAND
SECURITY
Federal Emergency Management
Agency
[Docket ID FEMA–2014–0002]
Changes in Flood Hazard
Determinations
Federal Emergency
Management Agency, DHS.
ACTION: Final notice.
AGENCY:
New or modified Base (1%
annual-chance) Flood Elevations (BFEs),
base flood depths, Special Flood Hazard
Area (SFHA) boundaries or zone
designations, and/or regulatory
floodways (hereinafter referred to as
flood hazard determinations) as shown
on the indicated Letter of Map Revision
(LOMR) for each of the communities
listed in the table below are finalized.
Each LOMR revises the Flood Insurance
Rate Maps (FIRMs), and in some cases
the Flood Insurance Study (FIS) reports,
currently in effect for the listed
communities. The flood hazard
determinations modified by each LOMR
will be used to calculate flood insurance
premium rates for new buildings and
their contents.
DATES: The effective date for each
LOMR is indicated in the table below.
ADDRESSES: Each LOMR is available for
inspection at both the respective
Community Map Repository address
listed in the table below and online
through the FEMA Map Service Center
at www.msc.fema.gov.
FOR FURTHER INFORMATION CONTACT: Luis
Rodriguez, Chief, Engineering
Management Branch, Federal Insurance
and Mitigation Administration, FEMA,
500 C Street SW., Washington, DC
20472, (202) 646–4064, or (email)
Luis.Rodriguez3@fema.dhs.gov; or visit
the FEMA Map Information eXchange
(FMIX) online at
www.floodmaps.fema.gov/fhm/fmx_
main.html.
SUPPLEMENTARY INFORMATION: The
Federal Emergency Management Agency
(FEMA) makes the final flood hazard
determinations as shown in the LOMRs
for each community listed in the table
SUMMARY:
below. Notice of these modified flood
hazard determinations has been
published in newspapers of local
circulation and ninety (90) days have
elapsed since that publication. The
Deputy Associate Administrator for
Mitigation has resolved any appeals
resulting from this notification.
The modified flood hazard
determinations are made pursuant to
section 206 of the Flood Disaster
Protection Act of 1973, 42 U.S.C. 4105,
and are in accordance with the National
Flood Insurance Act of 1968, 42 U.S.C.
4001 et seq., and with 44 CFR part 65.
For rating purposes, the currently
effective community number is shown
and must be used for all new policies
and renewals.
The new or modified flood hazard
information is the basis for the
floodplain management measures that
the community is required either to
adopt or to show evidence of being
already in effect in order to remain
qualified for participation in the
National Flood Insurance Program
(NFIP).
This new or modified flood hazard
information, together with the
floodplain management criteria required
by 44 CFR 60.3, are the minimum that
are required. They should not be
construed to mean that the community
must change any existing ordinances
that are more stringent in their
floodplain management requirements.
The community may at any time enact
stricter requirements of its own or
pursuant to policies established by other
Federal, State, or regional entities.
This new or modified flood hazard
determinations are used to meet the
floodplain management requirements of
the NFIP and also are used to calculate
the appropriate flood insurance
premium rates for new buildings, and
for the contents in those buildings. The
changes in flood hazard determinations
are in accordance with 44 CFR 65.4.
Interested lessees and owners of real
property are encouraged to review the
final flood hazard information available
at the address cited below for each
community or online through the FEMA
Map Service Center at
www.msc.fema.gov.
Chief executive
officer of community
Community map repository
Effective date of
modification
The Honorable Kenneth E. Gulley,
Mayor, City of Bessemer, 1800 3rd
Avenue, North Bessemer, AL 35020.
The Honorable David Carrington, Chairman, Jefferson County Commission,
716 Richard Arrington, Jr., Boulevard
North, Birmingham, AL 35203.
City Hall, Engineering Department, 1800 3rd Avenue North,
Bessemer, AL 35020.
Jefferson County Land Development Department, 716 Richard Arrington, Jr., Boulevard
North, Suite 260, Birmingham,
AL 35203.
March 13, 2014 ..............
010115
March 13, 2014 ..............
010217
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E:\FR\FM\13MYN1.SGM
13MYN1
Community
No.
]]>Agencies
[Federal Register Volume 79, Number 92 (Tuesday, May 13, 2014)]
[Notices]
[Pages 27323-27324]
From the Federal Register Online via the Government Printing Office [www.gpo.gov]
[FR Doc No: 2014-10892]
-----------------------------------------------------------------------
DEPARTMENT OF HEALTH AND HUMAN SERVICES
National Institutes of Health
Request for Information: The National Toxicology Program
Interagency Center for the Evaluation of Alternative Toxicological
Methods Requests the Nomination of Reference Chemicals
SUMMARY: The National Toxicology Program (NTP) Interagency Center for
the Evaluation of Alternative Toxicological Methods (NICEATM) requests
the nomination of reference chemicals, with supporting data, to be used
to validate in vitro metabolizing systems with the potential to
interact with estrogen receptors (ERs) or androgen receptors (ARs).
Specifically, a list of chemicals is needed to characterize the
usefulness and limitations of in vitro metabolizing systems for use in
conjunction with ER and AR transactivation tests.
DATES: The deadline for receipt of information is June 2, 2014.
ADDRESSES: Nominated reference chemicals and associated data should be
submitted electronically in Microsoft[supreg] Excel or Word formats to
niceatm@niehs.nih.gov. A Microsoft[supreg] Excel template for data
submission is available at https://ntp.niehs.nih.gov/go/41493.
FOR FURTHER INFORMATION CONTACT: Dr. Warren S. Casey, Director,
NICEATM; email: warren.casey@nih.gov; telephone: (919) 316-4729.
SUPPLEMENTARY INFORMATION:
Background
Endocrine-active substances (EAS) are chemicals that interfere with
normal endocrine hormone function by mimicking, blocking, or increasing
their actions, thereby possibly causing adverse health effects. United
States legislation (e.g., 7 U.S.C. 136, 110 Stat 1613) requires that
chemicals be tested for their ability to disrupt the hormonal systems
of mammals; prospective international legislative proposals may have
similar requirements. Chemicals found to test positive in vitro as EAS
may be in vivo endocrine disruptors. The lack of in vitro tools that
mimic in vivo metabolism is the main obstacle to implementation of in
vitro tools for EAS toxicity testing. Improved understanding of
metabolic capabilities and limitations of in vitro toxicity testing is
critical to:
Ensure that no potentially active metabolites are missed
Allow better interpretation of results
Accurately predict species-specific characteristics of
absorption, metabolism, and excretion
While there is a growing body of international in vitro test
guidelines addressing EAS mechanisms and modes of action, there are few
or no standardized methods to incorporate metabolic and toxicokinetic
aspects into these EAS in vitro tests to date. In vitro assays for EAS
should incorporate metabolic enzyme systems to better address the
relevance of EAS tests to in vivo adverse outcome pathways.
The Organization for Economic Co-operation and Development (OECD)
Validation Management Group-Non-Animal (VMG-NA) expert working group
develops internationally accepted non-animal test guidelines to support
various international regulatory needs for the hazard identification of
potential EAS. These test guidelines describe methods and approaches
capable of identifying potential EAS without the use of animals.
Consistent with its purpose of evaluating alternative methods for
testing chemicals and chemical products, NICEATM participates in the
VMG-NA.
Test guidelines for in vitro assays for ER activity have been
evaluated and accepted by international regulatory authorities; test
guidelines for in vitro AR activity assays are currently in
development. However, none of these in vitro EAS assays account for
whole animal metabolism. Further development of specific tests is
needed to optimize the use of in vitro metabolism with EAS assays.
Identification of appropriate reference chemicals to check the
metabolic capacity of any proposed test method is key to continued
assay development. For this purpose, the VMG-NA is developing a robust
list of chemicals that, when metabolized, act as ER or AR agonist or
antagonists.
Request for Information
On behalf of the VMG-NA, NICEATM requests nominations of chemicals
that can be used to characterize and validate in vitro metabolizing
systems for use in conjunction with in vitro tests for ER and AR
transactivation. Responses are requested from all interested parties,
including the research community, health professionals, educators,
policy makers, industry, and the public. Considerations for selection
of appropriate chemicals include the ability of a chemical to act as an
ER or AR agonist or antagonist and:
Potential for metabolism to make a chemical either more potent
(bioactivation) or less potent (detoxification)
Likelihood of metabolism occurring in relevant routes of
exposure and target organs
Likelihood of metabolism occurring over a range of doses:
Information on the ratio of the half maximal effective or inhibitory
concentration (EC50 or IC50, respectively) of parent to daughter
metabolites will be useful and there is a particular need for
information pertaining to substances where biotransformation yields a
very small or very large ratio of EC50/IC50 of parent to daughter
metabolites
Stability, preferably with real-time curves and consequent
exposure significance of likely metabolites
Diversity of likely and predominant biotransformative pathways
Diversity of chemical types, use classes, and consequent
applicability domains
The reference chemicals will be used to check the metabolic
capacity of the in vitro model, including characterization of the
general metabolic capacity of the cell lines. To ensure relevant use in
a regulatory context, it will be necessary, where possible, to make
correlations to:
(a) Relevant in vivo metabolic modeling (accounting for absorption,
distribution, metabolism, and excretion, etc.) of plasma/blood
metabolites in vertebrate animals (e.g., rat, fish, human).
(b) Data from the uterotrophic, Hershberger, and/or other relevant
assays with a demonstrated high confidence in prediction of
bioactivation of estrogenic or androgenic agonist and antagonist
pathways, such that the true systemic in vivo metabolic response is
addressed as accurately as possible.
When reporting the in vitro dose response for potential reference
chemicals, the concentrations of solvent and/or carrier proteins used
in the assay buffers to solubilize the reference chemicals should be
described to facilitate an understanding of potential differences among
new in vitro assays with regard to free concentrations of parent
chemical and metabolites versus nominal dosages within each testing
system.
Nominated reference chemicals and associated data should be
submitted electronically in Microsoft[supreg] Excel or Word formats to
niceatm@niehs.nih.gov. Data submitted can include, but need
[[Page 27324]]
not be limited to, citations of reports in the published literature,
data from past or ongoing validation studies, data in databases, or
unpublished data. A template for data submission is available at https://ntp.niehs.nih.gov/go/41493.
Responses to this request are voluntary. NICEATM does not intend to
publish a summary of responses received or any other information
provided. No proprietary, classified, confidential, or sensitive
information should be included in your response. Please note that the
U.S. Government will not pay for the preparation of any information
submitted or for its use of that information.
Those submitting information should include name, affiliation,
mailing address, phone, fax, email address, and sponsoring organization
(if any) with the submission. The deadline for receipt of the requested
information is June 2, 2014.
Background Information on NICEATM
NICEATM conducts data analyses, workshops, independent validation
studies, and other activities to assess new, revised, and alternative
test methods and strategies and provides support for the Interagency
Coordinating Committee on the Validation of Alternative Methods
(ICCVAM). The ICCVAM Authorization Act of 2000 (42 U.S.C. 285l-3)
provides authority for ICCVAM and NICEATM to conduct activities
relevant to the development of alternative test methods. Information
about NICEATM and ICCVAM is found at https://ntp.niehs.nih.gov/go/niceatm and https://ntp.niehs.nih.gov/go/iccvam.
Dated: May 7, 2014.
John R. Bucher,
Associate Director, National Toxicology Program.
[FR Doc. 2014-10892 Filed 5-12-14; 8:45 am]
BILLING CODE 4140-01-P
