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and Human Services (HHS)
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NETWORK FOR LARGE-SCALE SEQUENCING OF THE RAT GENOME
Release Date: July 17, 2000
RFA: HG-00-002
National Human Genome Research Institute
http://www.nhgri.nih.gov/
National Heart, Lung and Blood Institute
http://www.nhlbi.nih.gov/index.htm
Letter of Intent Receipt Date: August 15, 2000
Application Receipt Date: September 21, 2000
PURPOSE
This is a joint initiative between the NHGRI and the NHLBI to expand the current NHGRI
program for sequencing the rat genome. The goal of this program is to generate a
working draft version (3-4 fold sequence coverage) of the rat genome sequence in two
years or less. This announcement is intended to solicit proposals to accomplish two
of the sequencing elements of this program: light sequence coverage of individual BAC
clones, and whole genome shotgun sequencing.
HEALTHY PEOPLE 2010
The Public Health Service (PHS) is committed to achieving the health promotion and
disease prevention objectives of "Healthy People 2010," a PHS-led national activity
for setting priority areas. This Request for Applications (RFA), Network for Large-
Scale Sequencing of the Rat Genome, is related to several of the priority areas.
Potential applicants may obtain a copy of "Healthy People 2010" at
http://health.gov/healthypeople/.
ELIGIBILITY REQUIRMENTS
Applications may be submitted by domestic non-profit and for-profit organizations,
private and public, such as universities, colleges, private companies, hospitals,
laboratories, units of state or local governments, and eligible agencies of the
Federal government. Applications from foreign institutions will not be accepted;
however subcontracts to foreign institutions will be considered. Racial/ethnic
minority individuals, women, and persons with disabilities are encouraged to apply as
Principal Investigators.
The goals of this RFA can be met in a reasonable time frame only by groups that are
already sequencing at a significant scale. Therefore, applications will be accepted
only from organizations that have attempted at least 1,000,000 lanes of genomic
sequence data in the 12 months prior to the submission date.
MECHANISM OF SUPPORT
This RFA will use the National Institutes of Health (NIH) Cooperative Agreement, an
"assistance" mechanism which is distinguished from a regular research grant in that
substantial scientific and/or programmatic involvement by NHGRI and NHLBI staff with
the awardee is anticipated. The cooperative agreement is used when participation by
NIH staff is warranted to support and/or stimulate the recipient's activity by
involvement in and otherwise working jointly with the award recipient in a partner
role; NIH staff will not assume direction, prime responsibility, or a dominant role in
the activity. Details of the responsibilities, relationships, and governance of the
studies funded under cooperative agreement(s) are discussed later in this document
under the section "Terms and Conditions of Award". Applicants may apply for either a
new cooperative agreement (U01) or a competing supplement to an existing NHGRI
cooperative agreement (U01 or U54). This initiative will be managed by NHGRI staff
with input and the close cooperation of NHLBI staff.
The length of the project period is two years. The sizes of the awards will be
dependent upon the results of the peer review process. The anticipated award date is
January 1, 2001.
FUNDS AVAILABLE
It is estimated that up to $32 million (total costs) will be available to support the
first year of awards made in response to this RFA and up to $26 million (total costs)
for the second year of support. One to three awards will be made. In combination
with the amount of funds that NHGRI has already awarded to two centers to begin work
on this project, the total amount of funds should be adequate to support the
generation of the working draft sequence of the rat. The actual level of support will
be dependent on the receipt of a sufficient number of applications of high scientific
merit and the availability of funds. The funding level of each of the sequencing
centers will be subject to an annual evaluation by the Scientific Advisory Panel of
the Genome Sequencing Network (see below for details).
RESEARCH OBJECTIVES AND SCOPE
Background
The NHGRI is currently engaged, along with several other federal, private, and
international organizations, in a multi-year research program called the Human Genome
Project (HGP). Many of the initial goals of the HGP, including genetic and physical
maps of the mouse and human, and the DNA sequences of E. coli, S. cerevisiae, C.
elegans and D. melanogaster, have been realized. Significant progress has also been
made toward the sequencing of the human genome. By the end of June 2000, the public
sequencing effort had released approximately 85% of the genome in at least "working
draft" form, with more than 20% of the human sequence, including all of chromosomes 21
and 22, in finished form. The complete high quality human sequence will follow within
the next two to three years. Mouse genome sequencing has also begun; an intermediate
version of the mouse sequence will be generated within the next two years and the
complete sequence will follow no later than 2005 and probably much sooner.
As sequencing technology and efficiency have improved, the capacity of the world-wide
sequencing enterprise has increased substantially. Production sequencing capacity has
reached the point that one or a few large-scale centers can complete the sequencing of
an entire large genome in a short time. This presents an opportunity to sequence
multiple large genomes in parallel.
The availability of the genome sequence from three mammalian genomes would accelerate
the annotation of the human genome, since regions of evolutionary conservation between
the three genomes will help to identify protein coding sequences and other important
sequence features, such as regulatory regions. The rat genome is a clear choice to be
sequenced as the third model mammalian sequence as it has served as an important
physiological model for the human for many years. The NIH has already invested
significantly in generating genomic resources for the rat. In recognition of the
potential of rat models to contribute to the understanding of basic biology and human
health and disease, the NIH launched the Rat Genome Program in 1995, and the Rat EST
Program in 1997. In addition, the Rat Genome Database is now on line
(http://rgd.mcw.edu/). These three programs, led collaboratively by the NHLBI and
NHGRI, were funded by a number of Institutes and Centers at NIH and have produced a
variety of basic genomic resources for the rat. Obtaining the sequence of the rat
genome would bring nearly two hundred years of pharmacological, toxicological, and
physiological data from the rat into genomic context. The biological relevance and
wealth of phenotypic data in the rat, when combined with the current and proposed
genomic resources in mouse and human, would accelerate the development of new
diagnostic, prevention, and treatment approaches for human medicine. Recognizing the
value of obtaining the sequence of three mammalian organisms, the human, mouse and rat
as soon as possible, NHGRI and NHLBI have initiated the rat genome sequencing
initiative. Two NHGRI-supported sequencing centers have already begun a sequencing
effort to generate one-fold sequence coverage of the rat genome within the next year.
Research Scope
The initial goal of the Rat Genome Sequencing Project will be to generate a working
draft sequence (approximately 4-fold average sequence coverage) of 90% of the
euchromatic portions of the rat genome in two years. On the basis of lessons learned
during the sequencing of the human genome, the NHGRI wishes to evaluate a hybrid
sequencing strategy, involving both map-based and whole genome shotgun components, for
sequencing the mouse and rat genomes.
The map-based component of the hybrid strategy will consist of light sequence coverage
(about 1 fold) of a set of BAC clones covering the genome (the fingerprints and end
sequences of those clones will be funded separately and made publicly available). The
whole-genome shotgun sequence component, consisting of sequence derived from members
of a random shotgun library of the entire rat genome (e.g., paired plasmid-end
sequence) will represent the majority of the sequence data to be obtained. The hybrid
strategy is designed to quickly obtain a useful representation of the rat DNA
sequence, while facilitating the assembly of the whole genome shotgun sequence data
and its proper alignment along the chromosomal map. Applicants should submit
proposals to participate in the implementation and evaluation of the hybrid sequencing
strategy for the rat genome
This strategy requires a tightly focused, large-scale effort, involving no more than
two or three sequencing centers. In order to initiate the project rapidly and cost
effectively, only existing large-scale efforts are eligible to apply (see above). Once
the awards are made, the groups funded under this RFA, along with the NIH staff
participants in the cooperative agreements, will develop a collaborative plan to
produce the rat genome working draft sequence.
Applicants for production sequencing must address the items listed in Application
Guidance for Production Sequencing under Application Procedures.
NHGRI POLICIES CONCERNING DNA SEQUENCING
Over the past several years, NHGRI has established a number of policies related to
large-scale sequencing as described below. These policies will apply to all awards
made as a result of this RFA. Thus, where applicable, applicants must present plans to
adhere to the policies:
Intellectual Property. In NHGRI's opinion, in the absence of specific biological
information, genomic DNA sequence information should not be patented but released into
the public domain where it will be freely available for use by the entire research
community (see web site:
http://www.nhgri.nih.gov/Grant_info/Funding/Statements/RFA/intellectual_property.html)
Applicants are reminded that the grantee institution is required to disclose each
subject invention to the Federal Agency providing research funds within two months
after the inventor discloses it in writing to grantee institution personnel
responsible for patent matters (see http://www.iedison.gov/). NHGRI and NHLBI will
monitor adherence to this policy through the use of the appropriate existing
databases, to learn whether or not attempts are being made to patent large blocks of
primary rat genomic DNA sequence.
Data Release. In the case of the sequencing of the human, NHGRI policy encourages
grantees to release DNA sequence assemblies of 2,000 base pair units or larger within
24 hours of assembly (see http://www.nhgri.nih.gov/Grant_info/Funding/Statements/).
Participants in the international human DNA sequencing effort have recommended that
this policy be applied to sequence data from any organism (Genome Research, Vol. 8,
Issue 5, 413-413, May 1998). However, as currently stated, the policy is not
immediately applicable to sequence data generated from a whole genome shotgun project
because such data will not, early in the project, fall into the 2 kb contigs to which
the policy refers. NHGRI is currently consulting with a number of advisors, including
sequencers, sequence users, and the National Advisory Council for Human Genome
Research, to develop an extension of the policy that will continue to ensure the
public release of hybrid map-based/whole genome shotgun data on a similarly rapid
basis.
Sequence Quality. An important component of the HGP's sequencing program has been the
establishment of quality standards for sequence products, both finished and working
draft sequence. Just as important has been the assessment of sequence data produced
by the HGP participants. The standards and results of previous quality assessment
exercises are described at
http://www.nhgri.nih.gov:80/Grant_info/Funding/Statements/RFA/quality_standard.html.
NHGRI intends to assess the quality of the sequence data produced by the hybrid
strategy. However, the quality standards for a working draft determined by a hybrid
strategy will necessarily have to be modified from those previously established for
human working draft. Thus, as in the case of the data release policy, an extension of
the existing policy is needed and is currently being formulated. The assessment
criteria are likely to include read quality, data tracking, and assembly quality.
The quality of genomic data that a center has produced in the last year is likely to
be a reasonable general indicator of the quality of rat genome sequence that will be
produced, even if a different strategy (BAC by BAC) was used. Accordingly,
applicants should describe their experience in assessing the quality of their sequence
product (as described under special application guidance for production sequencing),
as well as discuss the results of recent NHGRI-conducted quality assessment of their
sequence data. If an applicant has not participated in an NHGRI-sponsored quality
assessment exercise, s/he should be prepared to submit data for independent analysis
during the review of their applications, if the reviewers request such information.
SPECIAL REQUIREMENTS FOR COOPERATIVE AGREEMENTS
I. Definitions
ARBITRATION PANEL: A panel that is formed to review scientific or programmatic
disagreement (within the scope of the award) that may arise between award recipients
and NHGRI and NHLBI. It will be composed of three members: (i) a designee of the
Steering Committee chosen without the NHGRI and NHLBI staff voting, (ii) one
NHGRI/NHLBI designee, and (iii) a third designee with relevant expertise who is chosen
by the other two (in the case of an individual disagreement, the first member may be
chosen by the individual awardee). The Arbitration Panel will help resolve both
scientific and programmatic issues that develop during the course of work and that
restrict progress.
AWARDEE: The institution to which the cooperative agreement is awarded.
COOPERATIVE AGREEMENT: An assistance mechanism in which there is anticipated
substantial involvement by NHGRI/NHLBI program staff with the recipient organization
during the performance of the planned activity.
GENOME SEQUENCING NETWORK: A group of scientists, each funded by a separate
cooperative agreement, working together to complete the DNA sequences of vertebrate
genomes. The Genome Sequencing Network currently is made up of extramural and NIH
intramural researchers involved in sequencing the human and mouse genomes.
NHGRI AND NHLBI PROGRAM DIRECTOR(S): Scientists of the NHGRI and NHLBI extramural
staffs who provide normal stewardship for the awards and who, in addition, have
substantial scientific/programming involvement during conduct of this activity, as
defined in the terms and conditions of award. The nature of this involvement is
described below.
PRINCIPAL INVESTIGATOR (P.I.): The person who assembles the project, is responsible
for submitting the application in response to this RFA, and is responsible for the
performance of the project. The Principal Investigator will coordinate project
activities scientifically and administratively.
STEERING COMMITTEE (SC): A committee that is the main governing board of the Genome
Sequencing Network. Membership includes the NHGRI and NHLBI Program Directors, the
P.I. of each awarded sequencing project, as well as the projects to characterize the
BAC libraries. Each cooperative agreement will have one vote. If needed,
subcommittees may be established to discuss issues that arise in the genome sequencing
of a specific organism.
SCIENTIFIC ADVISORY PANEL (SAP): A panel that evaluates the progress of the Genome
Sequencing Network and provides recommendations to the Director, NHGRI, about
continued support of the components of the Genome Sequencing Network. The Advisory
Panel is composed of four to six senior scientists with relevant expertise who are not
P.I.s of a cooperative agreement involved in the Genome Sequencing Network. A new
member will be jointly appointed to the SAP by the Directors, NHGRI and NHLBI, to
provide further advice on the rat genome sequencing project. If it is deemed
necessary, a subcommittee to the SAP may be appointed to deal with any specific issues
that might arise with the rat genome sequencing project. This subcommittee will be
appointed by the Directors, NHGRI and NHLBI.
II. Terms and Conditions of Award
The following terms and conditions will be incorporated into the award statement and
will be provided to the Principal Investigator, as well as the appropriate
institutional official, at the time of award. The following special terms of award
are in addition to, and not in lieu of, otherwise applicable OMB administrative
guidelines, HHS grant administration regulations at 45 CFR Parts 74 and 92 [Part 92 is
applicable when State and local Governments are eligible to apply], and other HHS,
NIH, and NIH grant administration policies:
1. The administrative and funding instrument used for this program will be the
Cooperative Agreement (U01, U54). The cooperative agreement is an "assistance"
mechanism (rather than an "acquisition" mechanism), in which substantial NIH
scientific and/or programmatic involvement with the awardee is anticipated during the
performance of the activity. Under the Cooperative Agreement, the NIH purpose is to
support and/or stimulate the recipient's activity by involvement in and otherwise
working jointly with the award recipient in a partner role, but it is not to assume
direction, prime responsibility, or a dominant role in the activity. Consistent with
this concept, the dominant role and prime responsibility for the activity resides with
the awardee(s) for the project as a whole, although specific tasks and activities in
carrying out the study will be shared among the awardee(s) and the NHGRI and NHLBI
Program Directors.
2. P.I. Rights and Responsibilities:
The P.I. will have the primary responsibility for defining the details for the project
within the guidelines of the RFA and for performing the scientific activity. The P.I.
will agree to accept close coordination, cooperation, and participation of NHGRI and
NHLBI staff in those aspects of scientific and technical management of the project as
described under "NHGRI and NHLBI Program Staff Responsibilities."
The P.I. of a sequence production center will:
o Determine experimental approaches, design protocols, set project milestones and
conduct experiments
o Ensure that the genomic sequence produced meets a quality standard and cost agreed
upon at the time of award
o Ensure that data resources developed as part of this project are released according
to NHGRI policies and that results are published and submitted to a public database
o Adhere to the NHGRI policies regarding intellectual property, data release and
other policies that might be established during the course of this activity
o Submit data for quality assessment in any manner specified by the Steering
Committee or the Scientific Advisory Panel.
o Submit periodic progress reports in a standard format, as agreed upon by the
Steering Committee and the Scientific Advisory Panel
o Accept and implement the common guidelines and procedures approved by the Steering
Committee
o Accept and participate in the cooperative nature of the group
o Attend Steering Committee meetings
o Coordinate and collaborate with other U.S. and international groups sequencing the
rat genome
3. NHGRI and NHLBI Program Staff Responsibilities:
The NHGRI and NHLBI Program Directors will have substantial scientific/programmatic
involvement during the conduct of this activity through technical assistance, advice
and coordination. However, the role of NHGRI and NHLBI will be to facilitate and not
to direct the activities. It is anticipated that decisions in all activities will be
reached by consensus of the Genome Sequencing Network and that NHGRI and NHLBI staff
will be given the opportunity to offer input to this process. One NHGRI and one NHLBI
Program Director shall participate as a member of the Steering Committee. Together,
NHGRI and NHLBI staff will have two votes. The Program Directors will:
o Participate (with the other Steering Committee members) in the group process of
setting research priorities, deciding optimal research approaches and protocol
designs, and contributing to the adjustment of research protocols or approaches as
warranted. The Program Directors will assist and facilitate the group process and not
direct it.
o Serve as liaison, helping to coordinate activities among and for the awardees,
including acting as a liaison to the NHGRI and NHLBI and the other Institutes and
Centers of the NIH, and as an information resource about extramural genome research
activities. The Program Directors will also coordinate the efforts of the Genome
Sequencing Network with other U.S. large-scale sequencing efforts and with the
international sequencing community.
o Attend all Steering Committee meetings as a voting member and assist in developing
operating guidelines, quality control procedures, and consistent policies for dealing
with recurrent situations that require coordinated action. The Program Directors must
be informed of all major interactions of members of the Steering Committee. The NHGRI
and NHLBI Program Directors will be responsible for scheduling the time and preparing
concise (3 to 4 pages) minutes or a summary of the Steering Committee meetings, which
will be delivered to members of the group within 30 days after each meeting. The
Program Directors will report progress to the NHGRI and NHLBI Directors, and other NIH
Institutes and Centers periodically.
o Lend relevant expertise and overall knowledge of NHGRI- and NHLBI- sponsored
research to facilitate the selection of scientists not affiliated with the awardee
institutions who are to serve on the Advisory Panel and the Steering Committee.
o Serve as liaison between the Steering Committee and the Advisory Panel, attending
Advisory Panel meetings in a non-voting liaison member role.
o Serve on subcommittees of the Steering Committee and the Advisory Panel, as
appropriate.
o Provide advice in the management and technical performance of the investigation.
o Assist in promoting the availability of the rat genome sequence and related
resources developed in the course of this project to the scientific community at
large.
o Retain the option to recommend the withholding or reduction of support from any
project within the Genome Sequencing Network that substantially fails to achieve its
sequencing goals at the quality and cost agreed to at the time of award, fails to
remain state of the art in its production sequencing capabilities, or fails to comply
with the Terms and Conditions of the award.
o Participate in data analyses, interpretations, and where warranted, co-authorship of
the publication of results of studies conducted through the Genome Sequencing Network.
4. Collaborative Responsibilities
The Steering Committee will serve as the main governing board of the Genome Sequencing
Network. The Steering Committee membership will include the NHGRI and NHLBI Program
Director(s), and the P.I. from each awarded cooperative agreement and intramural
project. Additional members may be added by action of the Steering Committee. Other
government staff may attend the Steering Committee meetings, if their expertise is
required for specific discussions. The National Center for Biotechnology Information
will maintain a central server to coordinate this project and will attend the Steering
Committee meetings. It will not be a member of the committee or have a vote.
The Steering Committee will be responsible for discussing progress within the Genome
Sequencing Network, and for advising NHGRI and NHLBI as to how the Genome Sequencing
Network can complete the working draft rat DNA sequence within the stated goals of
time and accuracy, and within budget. The Steering Committee will help to develop
uniform procedures for data quality assessment. Members of the Steering Committee will
be required to accept and implement the common guidelines and procedures approved by
the Steering Committee.
5. Scientific Advisory Panel
The Scientific Advisory Panel will be responsible for reviewing and evaluating the
progress of the Rat Genome Sequencing Network toward producing a working draft
sequence of the rat DNA sequence by 2002. The membership of the Scientific Advisory
Panel is described in the Definitions section, above. The membership of the Advisory
Panel may be enlarged permanently, or on an ad hoc basis, as needed.
The Scientific Advisory Panel will meet at least once a year. The first part of this
meeting will be a joint meeting with the Steering Committee to allow the Advisory
Panel members to interact directly with the members of the Genome Sequencing Network.
Annually, the Advisory Panel will make recommendations regarding progress of the
Genome Sequencing Network and present advice about changes, if any, which may be
necessary in the Genome Sequencing Network program to the Directors, NHGRI and NHLBI.
6. Arbitration Process
Any disagreement that may arise on scientific/programmatic matters (within the scope
of the award), between award recipients and the NHGRI and NHLBI may be brought to
arbitration. An Arbitration Panel, whose composition is described in the Definitions
(above) will be convened. This special arbitration procedure in no way affects the
awardee's right to appeal an adverse action that is otherwise appealable in accordance
with NIH regulations 42 CFR Part 50, Subpart D and HHS regulation at 45 CFR Part 16.
7. Yearly Milestones
All Awardees participating in the Genome Sequencing Network will be asked to define
yearly milestones at the time of the award and to update these milestones annually at
the anniversary date. These will be made a condition of the award. In accord with the
procedures described above, NHGRI and NHLBI may withhold or reduce funds for projects
that substantially fail to meet their milestones or to maintain the state of the art.
URLS IN NIH GRANT APPLICATIONS OR APPENDICES
All applications and proposals for NIH funding must be self-contained within specified
page limitations. Unless otherwise specified in an NIH solicitation, internet
addresses (URLs) should not be used to provide information necessary to the review
because reviewers are under no obligation to view the Internet sites. Reviewers are
cautioned that their anonymity may be compromised when they directly access an
Internet site.
LETTER OF INTENT
Prospective applicants are asked to submit a letter of intent that includes a
descriptive title of the proposed research, the name, address, and telephone number of
the Principal Investigator, the identities of other key personnel and participating
institutions, and the number and title of the RFA in response to which the application
may be submitted. Although a letter of intent is not required, is not binding, and
does not enter into the review of a subsequent application, the information that it
contains allows IC staff to estimate the potential review workload and plan the
review.
The letter of intent should be sent by August 15, 2000 to:
Dr. Jane L. Peterson
Program /Director, Large Scale Sequencing
National Human Genome Research Institute
National Institutes of Health
Building 31, Room B2B07, MSC2033
Bethesda, MD 20892-2033
APPLICATION PROCEDURES
The research grant application form NIH 398 (rev. 4/98) is to be used in applying for
these grants. These forms are available at most institutional offices of sponsored
research and may be obtained from the Division of Extramural Outreach and Information
Resources, National Institutes of Health, 6701 Rockledge Drive, MSC 7910, Bethesda, MD
20892-7910, telephone 301/710-0267, E-mail:GrantsInfo@nih.gov.
The RFA label available in the NIH 398 (Rev 4/98) application form must be affixed to
the bottom of the face page of the application. Type the RFA number on the label.
Failure to use this label could result in delayed processing of the application such
that it may not reach the review committee in time for review. In addition, the RFA
title and number must be typed on line 2 of the face page of the application form and
the YES box must be marked.
The sample RFA label available at:
https://grants.nih.gov/grants/funding/phs398/label-bk.pdf has been modified to
allow for this change. Please note this is in pdf format.
Submit a signed, typewritten original of the application, including the Checklist, and
three signed photocopies, in one package to:
CENTER FOR SCIENTIFIC REVIEW
NATIONAL INSTITUTES OF HEALTH
6701 ROCKLEDGE DRIVE, SUITE 1040 - MSC 7710
BETHESDA, MD 20892-7710
or BETHESDA, MD 20817 (for express/courier service)
At the time of submission, two additional copies of the application must also be sent
to:
Dr. Ken Nakamura
Scientific Review Administrator
Office of Scientific Review
Building 31, Room B2B37, MSC 2032
National Human Genome Research Institute
National Institutes of Health
Bethesda, MD 20982-2032
Telephone: (301) 402-0838
Applications must be received by September 21, 2000. If an application is received
after that date, it will be returned to the applicant without review. The Center for
Scientific Review (CSR) will not accept any application that is essentially the same
as one currently pending initial review, unless the applicant withdraws the pending
application. The CSR will not accept any application that is essentially the same as
one already reviewed.
SPECIAL APPLICATION GUIDANCE FOR PRODUCTION SEQUENCING
Applicants must consider and address the following in preparing applications for
sequence production projects called for in this RFA:
I. Progress Report
The NHGRI has conducted several competitions for large-scale sequencing projects
during the past few years. In so doing, it has been our experience that there are
specific information items that are central to the review of large-scale sequencing
proposals, and that the applications that have been most highly rated have provided
that information clearly and succinctly.
For the purposes of this RFA, completed data is defined as any genomic sequence data
produced in your center.
Section A. Text. The total length for this section should not exceed 10-15 pages
(5000-7500 words). Brief, concise answers are encouraged. Please focus these answers
on your past accomplishments, rather than future plans, unless specifically asked for.
1. Sequence production. How does your group's past effort support its ability to
successfully accommodate the rat sequencing project? Discussion should include, but is
not limited to:
Prior experience in sequencing and increasing throughput. What is the amount of
genomic sequence produced in the last year by your center? How much of that, if any,
was deposited in a public database? Based on an average of the last three months of
sequencing, what is the total current capacity of your group (include the number of
attempted lanes per month, the number of successful lanes per month, and the number of
base pairs per lane at of least phred 20--or equivalent--quality)? Please include
capacity from sequencing genomic DNA of other organisms and capacity due to funding
from all sources. If you have produced paired end reads from cloned inserts, describe
your experience in tracking the paired ends as well as your success in retrieving the
data. Applicant's experience, if any, in whole genome shotgun sequencing should be
described.
Prior experience in attaining milestones. What example(s) can you provide that you
have proposed milestones for a sequencing project and then met them on schedule? What
internal metrics have you used to evaluate progress in the past and what internal
metrics (for example, reads/month, failed lanes, base pairs per lane in GenBank, etc.)
do you believe will be the most useful to you in managing your project's sequencing
performance?
Cost analysis. What is your current cost per lane for shotgun sequence? Do you
anticipate being able to reduce that further in the next year? In the next two years?
If so, please explain how. You should express cost analyses in terms of total costs,
which include all equipment and indirect costs, as well as direct costs. How do you
monitor costs internally?
Integration. Do you anticipate that there will be any issues associated with
expanding your center's program to include sequencing the genome of a new organism? If
not, please explain why. If so, please discuss how those integration problems will be
addressed.
2. Discuss how your center checks the quality of the sequence it produces.
3. How do you expect your management plan to accommodate the needs of this project?
4. State your data release policy.
Section B. Graphical and Tabular Material
Please provide the following material.
1. A graph indicating, for the past year, the number of lanes attempted per week, the
number of successful lanes per week, and the weekly success rate.
2. Please provide a graph showing shotgun sequence output per month for at least the
last 12 months. (This should be a non-cumulative monthly total.)
II. Research Proposal
Sequence Production Plan. The applicant must present a plan to implement and evaluate
the hybrid map-based/whole genome shotgun strategy for sequencing the rat genome, and
propose milestones for achieving the proposed sequence production. This must
thoroughly discuss and justify the applicant's specific choices pertinent to all
phases of the sequence pipeline, starting with subcloning of BAC clones (for the map-
based arm) or production of a whole genome shotgun library (for the other arm) through
release of the sequence data to GenBank. The applicant should also discuss how the
data to be generated could be used to produce the finished rat sequence if such an
outcome were to be called for by the NHGRI and NHLBI. It will be important to discuss
potential bottlenecks or other problems that may be anticipated and how they will be
addressed. Finally a plan for assembly (including a description of computational
issues) of the whole genome shotgun and individual BAC data must be provided.
Sequence Cost. Both past (monthly costs for the first six months of 2000) sequencing
costs and projected costs for rat sequence production must be included. Costs should
reflect the production only of working draft quality sequence; it is not necessary to
include finishing costs. The calculated costs of sequencing (both prior and projected
sequencing costs) must take into account all of the expenses associated with working
draft sequence production, beginning with construction of a BAC subclone library or
whole genome shotgun library, through assembly of the working draft sequence to the
depth proposed and data submission. The total cost of sequencing must also include
any production-related technology development (see below) that has been or will be
supported by the project. However, the applicant must also provide a breakdown of
costs so that the reviewers can evaluate the contribution of different cost elements,
such as production-related technology development, to the reported total cost.
Sequence Quality: Applicants should describe existing quality assessment protocols and
an analysis of the quality of sequence produced in the period January through June
2000. Internal quality control programs should be described, including quality
assessment criteria. Evidence of the usefulness of such programs should be included,
as well as any changes being proposed for the rat sequencing project. Applicants must
also be prepared to submit sequence data produced in the last six months, including
sequence traces, success rates, and information about data tracking, prior to review
if NHGRI and the reviewers decide that data quality needs to be assessed in more
detail. This decision will be made after the application has been seen by the
reviewers. If an applicant's data have been evaluated by an NHGRI quality assessment
exercise in the past six months, this may be sufficient to fulfill this requirement.
Management Plan. The management of a sequencing center requires a significant
commitment by the P.I. of the project. A P.I. for a large-scale project is expected
to devote at least 30% effort to the project. If a P.I. is already devoting more than
30% effort to the existing center, an additional 10% effort should be committed to the
rat sequencing project. A description of how the rat sequencing project will be
integrated into the other sequencing activities of the center should be provided.
REVIEW CONSIDERATIONS
General Considerations
Upon receipt, applications will be reviewed for completeness by CSR and for
responsiveness by the NHGRI and NHLBI. Incomplete applications will be returned to the
applicant without further consideration. If NHGRI and NHLBI staff find that the
application is not responsive to the RFA, it will be returned without further
consideration.
Applications that are complete and responsive to the RFA will be evaluated for
scientific and technical merit by an appropriate peer review group convened by the
NHGRI and NHLBI in accordance with the review criteria stated below. As part of the
initial merit review, a process will be used by the initial review group in which
applications receive a written critique and undergo a process in which only those
applications deemed to have the highest scientific merit, generally the top half of
the applications under review, will be discussed, assigned a priority score, and
receive a second level review by the National Advisory Council for Human Genome
Research and by the National Heart Lung and Blood Advisory Council.
All applications will be judged on the basis of the scientific and technical merit of
the proposed projects and the documented ability of the investigators to meet the
RESEARCH OBJECTIVES of the RFA.
Review Criteria
The application must be directed toward attaining the programmatic goals as stated
under RESEARCH OBJECTIVES AND SCOPE. The following criteria will be used by peer
review groups to evaluate these applications:
o Likelihood that the project will produce a significant fraction of the rat genome
working draft sequence
o Prior experience and quality of the proposed plan for:
a) Producing high quality sequence data
b) Increasing sequence throughput
c) Decreasing sequencing costs
o Quality of the proposed plan for sequence production and identifying and solving
critical integration problems, including adequacy of the informatics activities.
o Sequence quality:
a) Merit of sequence quality assessment plans, including monitoring and minimizing
sequencing errors, and other QA/QC plans
b) Results from NHGRI sequence quality assessment exercises
o Track Record of the P.I. and other key personnel
o Quality of the center's existing management, including workflow, plans for further
scale-up to accommodate rat genomic sequencing, divisions of labor/responsibility
among components, coordination between components, appropriate staffing, training,
etc.
o Plans for release of data and resources developed through this project.
o Plans to coordinate efforts with other U.S. and international large-scale
sequencing groups and mapping efforts
o Availability of the facilities, resources, expertise and technology necessary to
perform the research, and the level of institutional commitment.
o Appropriateness of the proposed budget and time-line in relation to the proposed
research.
AWARD CRITERIA
Awards will be made on the basis of scientific and technical merit as determined by
peer review, including the significance of the projected contribution toward meeting
the NHGRI program goal of contributing to the completion of the rat genome working
draft DNA sequence by the year 2003, program needs and balance, data release and
intellectual property, and the availability of funds.
INQUIRIES
Written and telephone inquiries concerning this RFA are encouraged. The opportunity to
clarify issues or questions about the RFA from potential applicants is welcome.
Direct inquiries regarding programmatic issues to:
Dr. Jane L. Peterson (for sequencing)
Division of Extramural Research
National Human Genome Research Institute
National Institutes of Health
Building 31, Room B2B07 MSC 2033
Bethesda, MD 20892-2033
Telephone: (301) 496-7531
FAX: (301) 480-2770
E-mail:Jane_Peterson@nih.gov
Dr. Ken Nakamura (for review)
Scientific Review Administrator
Office of Scientific Review
National Human Genome Research Institute
National Institutes of Health
Building 31, Room B2B37, MSC 2032
Bethesda, MD 20982-2032
Telephone: (301) 402-0838
E-mail: Ken_Nakamura@nih.gov
Direct inquiries regarding fiscal matters to:
Ms. Jean Cahill
Grants Administration Branch
National Human Genome Research Institute
Building 31, Room B2B34, MSC 2031
Bethesda, MD 20892-2031
Telephone: (301) 402-0733
FAX: (301) 402-1951
E-mail:Jean_Cahill@nih.gov
Schedule
Letter of Intent Receipt Date: August 15, 2000
Application Receipt Date: September 21, 2000
Scientific Review Date: October/November, 2000
Advisory Council Date: December, 2000
Anticipated Award Date: January 1, 2001
AUTHORITY AND REGULATIONS
This program is described in the catalog of Federal Domestic Assistance No. 93.172.
Awards are made under the authority of the Public Health Service Act, Title IV, Part A
(Public Law 78-410, as amended by Public Law 99-158, 42 USC 241 and 285) and
administered under NIH grants policies and Federal Regulations 42 CFR Part 52 and 45
CFR Parts 74 and 92. This program is not subject to the intergovernmental review
requirements of Executive Order 122372 or Health Systems Agency review.
The NIH strongly encourages all grant and contract recipients to provide a smoke- free
workplace and promote the non-use of all tobacco products. In addition, Public Law
103-227, the Pro-Children Act of 1994, prohibits smoking in certain facilities (or in
some cases, any portion of a facility) in which regular or routine education, library,
day care, health care or early childhood development services are provided to
children. This is consistent with the NIH mission to protect and advance the physical
and mental health of the American people.
Return to NIH Guide Main Index
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