EXPIRED
It is critical that applicants follow the Multi-Project (M) Instructions in the SF424 (R&R) Application Guide, except where instructed to do otherwise (in this FOA or in a Notice from the NIH Guide for Grants and Contracts). Conformance to all requirements (both in the Application Guide and the FOA) is required and strictly enforced. Applicants must read and follow all application instructions in the Application Guide as well as any program-specific instructions noted in Section IV. When the program-specific instructions deviate from those in the Application Guide, follow the program-specific instructions. Applications that do not comply with these instructions may be delayed or not accepted for review.
Part 1. Overview Information
Part 2. Full Text of the Announcement
Section
I. Funding Opportunity Description
Section II. Award Information
Section III. Eligibility Information
Section IV. Application and Submission
Information
Section V. Application Review Information
Section VI. Award Administration Information
Section VII. Agency Contacts
Section VIII. Other Information
The vision for the Human BioMolecular Atlas Program (HuBMAP) is to catalyze development of a framework for mapping of the human body at high resolution to transform our understanding of tissue organization and function. This will be achieved by:
This program is funded through the NIH Common Fund as a short-term, goal-driven strategic investment, with deliverables intended to catalyze research across multiple biomedical research disciplines. The NIH Common Fund supports cross-cutting programs that are expected to have exceptionally high impact. All Common Fund initiatives invite investigators to develop bold, innovative, and often risky approaches to address problems that may seem intractable or to seize new opportunities that offer the potential for rapid progress.
The HuBMAP Consortium will scale-up the range of tissues, technologies, data management and its community engagement activities throughout the duration of the program.
The five research initiatives that compose the program are:
Understanding how tissue organization influences a cell s molecular state, interactions, and history is critical for enhancing our understanding of variation in organ function across the lifespan and health-disease continuum. Despite vastly improved imaging and omics technologies and many important foundational discoveries, our understanding of how tissues are organized is restricted to a very limited number of microscopic structures. Better insights into the principles governing organization-function relationship will potentially lead to better understanding of the significance of inter-individual variability, changes across the lifespan, tissue engineering, and the emergence of disease at the biomolecular level. However, integrating imaging and omics analysis to comprehensively profile biomolecular distribution and morphology of tissues in a high throughput manner and placing this information into 3D tissue maps amenable to modelling has yet to be fully realized.
In a June 2016 meeting (https://www.commonfund.nih.gov/sites/default/files/HuBMAP%20Summary%20of%20Planning%20Meeting.docx) organized by the NIH, experts from the research community identified the following scientific priorities necessary to develop these tissue maps: 1) sourcing high quality tissue from multiple human normal organ sites, 2) processing and preserving tissue for multiple imaging and omics assays, 3) quality control, validation and variation in data generation, 4) data coordination across multiple acquisition techniques, 5) annotation, curation and archiving of the data, 6) browsing, visualizing and searching the data, 7) building statistical and analytic techniques and models for nonlinear analysis of highly multidimensional data and 8) community engagement.
This FOA seeks to expand the number of state-of-the-art Tissue Mapping Centers (TMCs) in the HuBMAP Consortium to generate high-resolution, multi-parameter, 3D biomolecular maps of non-diseased human organs and organ systems not comprehensively studied by existing TMCs. Successful centers will build, benchmark, and standardize a pipeline for generating, validating and analyzing data from multiplexed, high-throughput imaging and omics technologies. Centers will be expected to integrate and optimize all parts of the data generation pipeline, from tissue collection and preservation through to data integration, analysis and interpretation in order to build these high-resolution maps. Centers will use these maps to provide new insights into intra-, inter- and extra- cellular organizational features that influence tissue function, vary across individuals or that change across the lifespan. By the end of four years of funding, a successful center will have created a significant number of high-resolution, multi-scale, multi-dimensional molecular, cellular and morphological maps for multiple organs and donors.
Centers funded by the FOA will be expected to work closely with the existing HuBMAP Consortium and to nimbly and rapidly harmonize their workflows with existing SOPs. However, new Centers should clearly distinguish themselves from existing projects funded by NIH or other funding organizations in their goals, tissues, assays and personnel to avoid any perception of overlap. Centers are expected to propose an array of assays, which through integrated analysis, will significantly enhance understanding of the spatial distribution of many biomolecules. Higher programmatic priority will be given to applications that propose to study complete human organs not currently studied by existing TMCs, that propose a synergistic set of assays for multiscale and multi-modal analysis and that have approved informed consent from donors or their families for explicit sharing of genomic data. For further information about the HuBMAP Consortium, please see: https://commonfund.nih.gov/hubmap.
The success of HuBMAP is dependent on building a community resource that can be utilized easily and effectively by the wider research community. All TMCs are expected to generate resources, such as high-quality data, metadata, software or protocols, and to make these rapidly and openly available for use by the Consortium and research community. Making data, metadata, software and other digital objects open, findable, accessible, interoperable, and reusable (FAIR) and citable and for those datasets to be rigorous and reproducible are critical to the success of the program. In order for TMCs to get up and running quickly, applicants are strongly encouraged to optimize or adapt appropriate existing tissue collection protocols, assays, and analytical methods and to create new ones only when required. Applicants are also strongly encouraged to optimize or adapt solutions from other communities that have tackled similar mapping challenges. New Centers can propose partnering with existing Consortium members or be composed or to partner with funded groups in the wider international atlas-building ecosystem, however if they do so they should provide a compelling explanation of why no overlap exists.
NIH expects to fund at least one Center focused in each of the following areas: 1) analysis of multiple discrete, complex organs from the same individual or a region of the body composed of multiple tissues, 2) analysis of a complete organ or system and 3) analysis of rare, dynamic or motile cell types and their microenvironments or tissue neighborhoods. Accordingly, applicants should be cognizant that a subset of proposed Organ Specific Projects may be funded based on programmatic priorities, and that Organ Specific Projects (OSPs) from multiple TMCs may be expected to work closely together around large, complex organs or systems. Further, programmatic priority will be given to Centers proposing to study tissues and organs not currently funded under the existing RFA-RM-17-027 (see: https://commonfund.nih.gov/HuBMAP/fundedresearch).
This FOA encourages applicants to propose strategies that include but are not limited to addressing the following challenges:
Applications addressing the following topics will be deemed non-responsive and will not be reviewed:
Centers should have a clear vision and detailed plan for mapping multiple non-diseased human organs and tissues during the funding period. Applicants must be able to perform comprehensive characterizations of the quality of human biospecimens at high resolution and describe plans for biospecimen management, quality control and minimization of tissue degradation. During the first year of funding, Centers are encouraged to start by building high quality tissue repository, optimizing and harmonizing their pipeline, benchmarking their assays and ensuring data is interoperable with the rest of the Consortium. After the first year, projects are expected to define data generation milestones every 6 months. For each new tissue and organ, a TMC is expected to take the lead for establishing best practices for collection and preservation of that tissue while building on the knowledgebase already developed by the wider community.
The TMCs collectively establish Consortium-wide best-practices for collection and preservation of tissues for tissue quality control and assembly of specimen metadata for downstream interrogation and analysis. Centers are strongly encouraged to plan a prospective collection strategy, including collecting appropriate epidemiological and anatomical data alongside data on specimen collection to ensure data can be integrated through the Common Coordinate Framework for intra- and inter-individual comparisons and an integrated view of the whole body. Centers may also propose including a minority of work with retrospective samples where the quality and provenance are well established through preliminary results. Centers are strongly encouraged to identify robust biological and statistical rationales for sampling decisions from non-diseased human donors, for example whether to focus on intra-individual sampling, inter-individual sampling across the lifespan or within a genetic group, or temporal sampling.
Centers are strongly encouraged to develop enrollment criteria and acquisition strategies that will minimize the risk of abnormal or degraded tissue as part of a quality management strategy. Applicants are also strongly encouraged to pursue explicit consent from the donor or their family for unrestricted sharing of data for research purposes to maximize the utility of biospecimens and data and to make sure their institutional policies are consistent with the Consortium's Data Use and Material Transfer Agreements (see: https://hubmapconsortium.org/policies/). Teams are encouraged to have strong scientific justification for their choice of tissues and to consider availability of high-quality tissue, synergies with other initiatives, and matching technical expertise of specific tissues with general technology capabilities. Applicants are also encouraged to consider Ethical, Legal and Social Issues (ELSI) of tissue collection and to consider return of results to donors or their families. Programmatic priority will be given to Centers with established informed consent from a diverse range of donors or their families for explicit sharing of genomic data.
Centers should anticipate working closely with the rest of the consortium around biospecimens. TMCs are expected to collaborate closely with each other by sharing biospecimens, protocols and data. In addition, they should anticipate working closely with the HIVE on the coordination and tracking of biospecimens using the Consortium’s UUID system along with standardizing clinical and collection metadata, collecting tissues consistent with the needs of the Common Coordinate Framework and on the formats and annotations required for successful data submission to the archive. TMCs are also expected to collaborate closely with the TTD and RTI projects to provide a testbed for validating emerging technologies.
HuBMAP projects will generate high resolution, high content, high-throughput biomolecular data to generate 3D tissue maps of non-diseased human organs and organ systems. For HuBMAP, a high-resolution assay is one that can reliably and reproducibly assign detected biomolecules to individual cells or extracellular compartments of a tissue. A high content approach is one that maximizes identification of tissue features through a combination of biomolecular depth, spatial resolution and multiplexing of complementary, multi-parameter assays. A high throughput pipeline is one that maximizes the bandwidth of data production to result in any or all of the following: 1) accelerated speed of analysis, so that hundreds or thousands of samples can be analyzed simultaneously, 2) greater depth of analysis, so that hundreds or thousands of molecules can be analyzed in a single sample, or 3) enhanced capacity for volume, so that a given set of molecules can be analyzed in all the cells within a larger tissue sample. Programmatic priority will be given to approaches that maximize the volume of tissue that will be analyzed while maintaining cellular resolution and high biomolecular content.
Given the focus of HuBMAP on spatial analysis, proposed assays must be capable of defining location at high resolution, provide comprehensive insight into the distribution of multiple biomolecules, and be applied to multiple human tissues. This FOA seeks to utilize high resolution, high-content, high-throughput, cost-effective assays that generate high quality quantitative data for characterizing cells and the extracellular structures at high resolution, which at the same time allows the capture of position and orientation information within the tissue and within the human body. The combination of these assays must be capable of robustly characterizing all the cells of human origin present in the tissues and their extracellular environment. Centers are expected to be able to characterize the spatial distribution of a significant number and variety of biomolecules using established techniques such as FISH, immunofluorescence, imaging mass spectrometry and sequencing, and are strongly encouraged to incorporate, optimize and validate emerging in situ assays that will generate complementary quantitative, high-content, high-throughput biomolecular data. The vision for the Center, the choice of tissues to be analyzed and technical expertise should be used to justify the choice of assays employed. Although most of the work proposed by the TMC should be on in-situ analysis of the biomolecular composition and morphology of tissue, it is accepted that a minority of work on unbiased, dissociative techniques can be used to inform the in-situ analysis in an iterative fashion. Likewise, although the focus is on building quantitative biomolecular tissue maps of human tissues, TMCs can propose pipelines that integrate data sources that will enhance scientific understanding, including from but not limited to MRI, micro-CT, photoacoustic imaging, Raman spectroscopy, histology stains, and mechanical imaging. Programmatic priority will be given to Centers proposing a synergistic set of well-validated assays for multiscale and multi-modal analysis of large volumes of tissue.
Central to the purpose of the TMCs is the construction of high-resolution 3D maps of human tissues containing molecular, cellular, and tissue-level spatial, functional, and/or temporal relationships that are searchable and scalable. The Center is expected to develop computational tools and analytical workflows that will facilitate map construction through the generation, visualization and modelling of multi-dimensional maps from their proposed high-content, multiparameter imaging and omics assays. Applicants should propose to use methods that have been demonstrated to generate high-quality data, to fuse data types together for joint analysis, to validate segmentation and definition of cell types and to test the rigor, reproducibility and robustness of data, algorithms and models.
Making data, metadata, software and other digital objects open, findable, accessible, interoperable, and reusable (FAIR) and citable especially as our understanding of these concepts evolve over time are key to the success of the HuBMAP. Applicants are strongly encouraged to propose using modular and scalable solutions where information and data exchange with the HIVE is formalized using standard (and fully open) file formats; using Application Programming Interfaces (APIs) and standards like RESTful; adopting suitable Workflow languages; containerization for reproducibility, etc. Applicants are strongly encouraged to discuss their proposed projects with the HIVE (please see: https://commonfund.nih.gov/hubmap/fundedresearch) in advance of submitting their application to understand the current file formats, metadata schemas, clinical data and data submission process, so they can articulate how their approach is open and modular in nature and consistent with current HIVE practices. Applicants are strongly encouraged to optimize or adapt existing standards and approaches and to create new ones only when required. Applicants are also strongly encouraged to optimize or adapt solutions from other communities that have tackled similar mapping challenges.
Data security encompasses confidentiality, data integrity, and availability. All three elements are important for the HuBMAP and TMCs and maintaining confidentiality of controlled access data is a particularly high priority. Confidentiality includes managing data access to maintain data security and make data accessible to authorized users only for authorized purposes. Data security protection and proper stewardship of human genomic, phenotypic and other sensitive information stored and distributed by the TMCs is of the utmost importance. The Notice for Use of Cloud Computing Services for Storage and Analysis of Controlled-Access Data Subject to the NIH Genomic Data Sharing (GDS) Policy (Ref: https://grants.nih.gov/grants/guide/notice-files/NOT-OD-15-086.html) allows investigators to perform genomic analyses on a cloud platform. The NIH security best practices and provisions (https://www.ncbi.nlm.nih.gov/projects/gap/pdf/dbgap_2b_security_procedures.pdf) should be implemented to protect the privacy and confidentiality of research participants, and prevent unauthorized access to data. The applicant(s) are also expected to develop policies and procedures for notifying NIH staff, and managing, and mediating any loss of data or compromise of data confidentiality. Centers should conduct regular audits of its data security and protection processes, which should be validated by third party independent assessments. The Precision Medicine Initiative's Data Security Principles Implementation Guide provides an example for auditing and data security protection processes https://www.healthit.gov/sites/default/files/pmi_security_ig_v16-clean.pdf. Funded TMCs must adopt the current data sharing policies and data use agreements of the Consortium (see: https://hubmapconsortium.org/policies/), and take other steps to protect the privacy of research participants while at the same time making data rapidly available.
Successful applicants to this FOA will become members of the larger HuBMAP Consortium composed of investigators who have been funded in response to at least one of HuBMAP FOAs. The purpose of the Consortium is to enable groups to effectively collaborate with each other to maximize the chances of overall success of the program. In addition to completing the research goals outlined in their applications, successful applicants will be expected to work collaboratively with all members of the Consortium to contribute to developing SOPs, data and metadata standards, metrics for data generation, participate in cross-site studies, engage in cross-training, and guide development of data analysis and visualization tools that can be used by the broader scientific community. Further information about the Consortium can be found on their website: https://hubmapconsortium.org/.
A Steering Committee (SC) composed of all the funded principal investigators and NIH staff meets monthly to develop and implement Consortium policies and guide overall direction of the Consortium to meet the goals of the program. This Steering Committee is complemented by an Executive Committee and a set of working groups. NIH staff have also recruited outside experts (non-awardees) as External Program Consultants (EPCs) to provide advice directly to NIH. New HuBMAP investigators will be expected to abide by existing and future policies agreed on by the HuBMAP Steering committee, including data and metadata standards, data, formats and procedures for publication.
As the primary source of data in the Consortium, the TMCs are expected to work closely together to establish best practices for data generation, carryout cross-site comparisons and engage in joint analysis activities. TMCs will need to work closely with each other and the HIVE to: (1) make sure their pipelines are interoperable, reproducible and meet the goals of the Program and policies of the Consortium, (2) that the data from the assays can be integrated and aligned across using a Common Coordinate Framework, and (3) collaborate with other Consortium projects and the wider research community on QA/QC, standards, ontologies and to respond to community feedback. They are also expected to work closely with the HIVE to develop and implement data and metadata standards, develop the framework for building an integrated atlas that integrates all the maps in the context of the human body, and making data generated by the Consortium interoperable and reusable. TMCs are strongly encouraged to reuse and adapt existing and widely-used data and metadata standards, ontologies, schemas, and formats, and to use common data elements, machine readable formats, structured reports and to minimize human data entry where possible. It is envisaged that TMCs will consist of a highly multidisciplinary team with expertise in areas including, and is not limited to: pathology, clinical and microscopic imaging, image analysis, sequencing, molecular and cellular biology, bioinformatics, data science, biostatistics, systems biology, and mathematical modeling.
Given their central role in the Consortium, TMCs are encouraged to plan for mobility of researchers within the Consortium, either hosting researchers from other sites, or travelling to other sites to enhance collaboration. TMCs should also be prepared to work closely with the Rapid Technology Integration and Transformative Technology Development projects to develop, test and potentially integrate innovative technologies into their production pipelines. In addition, all HuBMAP investigators will also be required to attend the annual HuBMAP investigator meetings, regular teleconferences with Consortium members and NIH Staff for the duration of the funding cycle. Therefore, TMCs are asked to plan and budget for approximately 20% of their total budget for collaborative activities as part of their applications. These collaborative activities may include benchmarking of similar methods across sites, comparison of adjacent tissue slices by complementary methods, development of common analytical pipelines or joint analysis of data from the same tissue across multiple donors. Applicants are encouraged to include details of potential activities as part of their applications, however the final set of activities will be determined post-award through discussion with Consortium members and NIH staff.
NIH intends that the products of the TMCs be broadly available to the research community to establish the foundations for a human body map that other programs and the international community to build upon; this includes methods, tools, reagents, biospecimens, datasets, and software. Centers will be expected to abide by Consortium policies such as assay and data standards; the rapid sharing of sharing data, methods, and standards; publication of data and results; partnerships and participation of similar projects and programs and sharing of resources. Milestones for biospecimens collection and data generation will be recognized once details have been submitted to the HIVE. The robustness and reproducibility of experimental results are critical to the success of HuBMAP. In some cases, conducting additional critical experiments will be important for assessing progress. Therefore, NIH Program staff, in consultation with the PD/PI, may modify or add experiments to be conducted during the duration of an award.
This FOA uses the multicomponent U54 mechanism. Each TMC will be composed of a Coordination Core (CC), a Data Analysis Core (DAC) and up to three Organ Specific Projects (OSPs), one for each tissue type proposed. Centers are encouraged to consider staggering the introduction of these projects to scale based on prior experience, preliminary results, resources and personnel, and synergy with other projects. Each core and project should have a well-defined and distinct function as described below and be synergistic without being highly inter-dependent. The cores and projects may vary in size, start date and composition depending on the needs of the project, but should be integrated to achieve the overall goal of the Center. The proposed budget should reflect the needs of the Center, though is expected to scale-up as the center generates more data. Center staff should have a strong track-record of producing high-quality data as part of a consortium and with the tissues chosen as the focus of the OSPs.
Coordination Core: The Coordination Core (CC) will be responsible for general administrative duties and for coordinating activities within the TMC and sharing expertise and resources with the other TMCs. The CC will also be responsible for ensuring coordination with the HuBMAP Consortium and the wider research community. Data production by TMCs will be assessed for meeting goals and milestones at two-time points: 1) the point at which data passes QC metrics and is accepted for ingestion by the HIVE, and 2) data release to the research community. Likewise, biospecimen collection, preservation and quality management will be assessed in an analogous way. The leadership of the CC is responsible for ensuring relevant expertise is engaged at the appropriate time to meet the Center's goals and milestones. As part of their goals and milestones, TMCs should develop specific, quantitative, six-month milestones for collecting biospecimens, data generation, quality assessment and submission of data and metadata. The CC will also manage intra-and extra-consortium collaboration projects. Due to the highly multidisciplinary nature of these Centers and the focus on collaboration and expertise sharing, in addition to the PD/PIs, each Center must have a Program Manager with demonstrated experience and the ability to manage day-to-day aspects of the Center and understand diverse needs, people and projects.
Data Analysis Core: The Data Analysis Core (DAC) will be responsible for data annotation, curation, and analysis of data generated by the Center. The DAC will be responsible for building 3D tissue maps from the data generated by the Organ Specific Projects, including the registration of the data with respect to anatomical references, image segmentation and analysis, identification and annotation of cell types and states and extracellular compartment, and preparing different data sets for sharing. The DAC will share these maps and underlying data with the HIVE, to enable it to build an atlas of maps in the context of the whole human body. The DAC is strongly encouraged to use existing software packages and analysis methods, such as R-based or Python-based solutions, that would enhance reproducibility and re-use where possible, and consideration should be given to containerize the entire pipeline. The DAC will work closely with the CC to submit data and metadata in common, interoperable formats to the HIVE so that it can be easily integrated and re-used. The DAC will also work with the HIVE to optimize its secondary analysis pipelines and the implementation of a Common Coordinate Framework and with the other TMCs and the HIVE to implement Consortium-wide open, data and metadata standards and schemas; data quality metrics, ontologies and data elements; integration of imaging and omics data; analytical tools for visualization, segmentation and annotation. Responsibilities of DAC include ensuring that data is collected and submitted to the HIVE conforming with the agreed policies and practices of the Consortium, including Standard Operating Procedures (SOPs), data and metadata format and standards, the use of Common Data Elements (CDEs) and the Consortium's data sharing policy. DACs are strongly encouraged to propose using modular and scalable solutions where information and data exchange with the HIVE is formalized using standard (and fully open) file formats; using Application Programming Interfaces (APIs) and standards like RESTful; adopting suitable Workflow languages; containerization for reproducibility, etc. Applicants are strongly encouraged to talk with the HIVE Infrastructure and Engagement Center to understand how their approaches fit with the current architecture.
Organ Specific Project: An Organ-Specific Project (OSP) will be responsible for generating high quality tissue maps using multiple assays for one organ or component of an organ system. A Center can propose up to three distinct and synergistic OSPs, with each focused on a separate organ or component of an organ system. These responsibilities include establishing and optimizing SOPs for collection, preservation and quality control of tissue; collecting relevant metadata including location and orientation of biospecimens; validation and benchmarking of assays; and generating high quality, high-content spatial data using multiple assays with metrics for data quality control, reproducibility, and normal variation. Assays should be capable of high-resolution, state-of-the-art molecular, cellular, and tissue-level characterization of biospecimens for the purpose of constructing multi-scale, multi-dimensional tissue maps. The OSPs are expected to set up a framework for collecting high quality biospecimens in a consistent manner from human donors with a strong rationale for the sampling approach and collection of appropriate metadata that will enhance the utility of data. In order to maximize the utility of data generated by the Consortium, TMCs are strongly encouraged to have or to rapidly establish consents during the setup phase that (a) explicitly allow for open (non-restricted) data sharing for research, and (b) allow for sharing biospecimens with other HuBMAP-funded groups. The OSPs will also work closely with the Data Analysis Core (DAC) on topics such as providing data in consistent formats, with enough metadata describing the origin and nature of the biospecimen, details of collection and pre-analytical processing, details of the assays performed, and any filtering of the data prior to map generation. The OSPs in conjunction with the CC will also work closely with the HIVE later in the program to manage biospecimens, OSPs in other TMCs on SOPs, and the HIVE and the DACs on data and metadata standards and file formats. The OSPs needs to be flexible in their data collection strategies such that new technologies introduced through technology development projects, or related atlas building projects might be quickly tested, validated and adopted over the course of the award lifetime.
All applicants are strongly encouraged to contact NIH Staff to discuss the alignment of their proposed work with the goals of this FOA and the HuBMAP Program. A Technical Assistance teleconference will be held for potential applicants from 1-2pm Eastern Time on January 13, 2020. NIH staff will be available to answer questions related to this FOA. Dial in information for the call is posted on the HuBMAP website and slides will be made available on the website for those unable to attend. A list of frequently asked questions (FAQs) related to the program are also posted on the website: https://commonfund.nih.gov/hubmap/generalfaqs. The information session is open to all prospective applicants, but participation is not a prerequisite to apply.
See Section VIII. Other Information for award authorities and regulations.
NIH grants policies as described in the NIH Grants Policy Statement will apply to the applications submitted and awards made from this FOA.
Higher Education Institutions
The following types of Higher Education Institutions are always encouraged to apply for NIH support as Public or Private Institutions of Higher Education:
Nonprofits Other Than Institutions of Higher Education
For-Profit Organizations
Governments
Other
Non-domestic (non-U.S.) Entities (Foreign Institutions) are not eligible to apply.
Non-domestic (non-U.S.) components of U.S. Organizations are not eligible to apply.
Foreign components, as defined in the NIH Grants Policy Statement, are allowed.
Applicant Organizations
Applicant organizations must complete and maintain the following registrations as described in the SF 424 (R&R) Application Guide to be eligible to apply for or receive an award. All registrations must be completed prior to the application being submitted. Registration can take 6 weeks or more, so applicants should begin the registration process as soon as possible. The NIH Policy on Late Submission of Grant Applications states that failure to complete registrations in advance of a due date is not a valid reason for a late submission.
Program Directors/Principal Investigators (PD(s)/PI(s))
All PD(s)/PI(s) must have an eRA Commons account. PD(s)/PI(s) should work with their organizational officials to either create a new account or to affiliate their existing account with the applicant organization in eRA Commons.If the PD/PI is also the organizational Signing Official, they must have two distinct eRA Commons accounts, one for each role. Obtaining an eRA Commons account can take up to 2 weeks.
Any individual(s) with the skills, knowledge, and resources necessary to carry out the proposed research as the Program Director(s)/Principal Investigator(s) (PD(s)/PI(s)) is invited to work with his/her organization to develop an application for support. Individuals from underrepresented racial and ethnic groups as well as individuals with disabilities are always encouraged to apply for NIH support.
For institutions/organizations proposing multiple PDs/PIs, visit the Multiple Program Director/Principal Investigator Policy and submission details in the Senior/Key Person Profile (Expanded) Component of the SF424 (R&R) Application Guide.
This FOA does not require cost sharing as defined in the NIH Grants Policy Statement.
Applicant organizations may submit more than one application, provided that each application is scientifically distinct.
The NIH will not accept duplicate or highly overlapping applications under review at the same time. This means that the NIH will not accept:
The application forms package specific to this opportunity must be accessed through ASSIST or an institutional system-to-system solution. A button to apply using ASSIST is available in Part 1 of this FOA. See your administrative office for instructions if you plan to use an institutional system-to-system solution.
It is critical that applicants follow the Multi-Project (M) Instructions in the SF424 (R&R) Application Guide, except where instructed in this funding opportunity announcement to do otherwise and where instructions in the Application Guide are directly related to the Grants.gov downloadable forms currently used with most NIH opportunities. Conformance to the requirements in the Application Guide is required and strictly enforced. Applications that are out of compliance with these instructions may be delayed or not accepted for review.
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.
By the date listed in Part 1. Overview Information, prospective applicants are asked to submit a letter of intent that includes the following information:
The letter of intent should be sent to:
Zorina Galis, Ph.D.
Telephone: 301-435-0560
Email: [email protected]
Available Component Types |
Research Strategy/Program Plan Page Limits |
Overall |
6 |
Admin Core (use for Coordination Core) |
6 |
Core (use for the Data Analysis Core) |
6 |
Project (use for each Organ Specific Project) |
12 |
Additional page limits described in the SF424 Application Guide and the Table of Page Limits must be followed.
The following section supplements the instructions found in the SF424 (R&R) Application Guide, and should be used for preparing a multi-component application.
The application should consist of the following components:
When preparing your application, use Component Type Overall .
All instructions in the SF424 (R&R) Application Guide must be followed, with the following additional instructions, as noted.
Complete entire form.
Note: Human Embryonic Stem Cell lines from other components should be repeated in cell line table in Overall component.
Follow standard instructions.
NIH intends to fund an estimate of 4-6 awards, corresponding to a total of approximately $4M, for fiscal years 2020 and 2021, and $8M for fiscal years 2022 and 2023. The number of awards is contingent upon NIH appropriations and the submission of a sufficient number of meritorious applications.
Enter primary site only.
A summary of Project/Performance Sites in the Overall section of the assembled application image in eRA Commons compiled from data collected in the other components will be generated upon submission.
Include only the Project Director/Principal Investigator (PD/PI) and any multi-PDs/PIs (if applicable to this FOA) for the entire application.
A summary of Senior/Key Persons followed by their Biographical Sketches in the Overall section of the assembled application image in eRA Commons will be generated upon submission.
The only budget information included in the Overall component is the Estimated Project Funding section of the SF424 (R&R) Cover.
A budget summary in the Overall section of the assembled application image in eRA Commons compiled from detailed budget data collected in the other components will be generated upon submission.
Specific Aims: The Specific Aims should be overarching, visionary and distinct from the aims of the individual components.
Project Summary/Abstract: Provide an overview of the competitive advantages of the Center. Describe the vision and goals of the Center and how these contribute to accomplishing the overall goals of HuBMAP. Succinctly describe the tissue maps that will be generated and how they are synergistic with currently funded research.
Project Narrative: State how the maps constructed within the Center will further knowledge of the relationship between tissue organization and function and the potential impact this may have on public health. Briefly describe the relevance of the research products and resources to be generated by the Center activities for HuBMAP and the wider research community.
Research Strategy: The applicant must provide details of the center's vision and organization at a high level. In lieu of the standard Research Strategy sub-sections (Significance, Innovation, Approach), use the sub-sections defined below to present a concise overall vision and plan for the proposed TMC.
Center Research Strategy: Description and rationale for the major theme and structure of the Center, its goals and objectives, synergy with ongoing research and background information to provide feasibility of accomplishing these goals. The rationale and inter-connectedness between the tissues and organs chosen, the assays deployed, and between the cores and projects composing the Center should be clearly articulated. Describe the timeline and key milestones for the Center, highlighting when each Organ Specific Project will start and the rationale for this timing. Describe innovative aspects of the assays and how they will be integrated together for tissue mapping. Outline the significance and impact provided by the creation of these tissue maps and how the range of tissues and technologies will be expanded during the project. In addition, a vision for coordination and collaboration with the HuBMAP Consortium, as well as the greater research community and other key stakeholders must be described. Describe synergies and possible collaborations with other initiatives or the wider research community that would enhance the productivity of the Center. This FOA is not intended to support the development of new technologies, assays or models that are not well validated in mammalian tissues. However, because new and more powerful technologies are constantly emerging, describe a roadmap and methods for potentially incorporating them in later years.
Center Management Strategy: Without duplicating information in the biosketches, applicants should provide evidence of successful management of large, multi-component programs and prior experience with generating significant, high quality, imaging and omics data as part of a Consortium. In addition, the overall strategy should describe how the skills of individual team members will translate into the collective capability of the center, how the team brings complementary multidisciplinary scientific expertise required for the integration of multidimensional, multiparametric data and how the diverse expertise of the team members increases the capability for innovation, the ability to anticipate new directions, and the flexibility to redirect research when needed.
Goals and Milestones: Applicants should define a clear set of bi-annual (6-month) milestones for the proposed project that are consistent with the goal of developing widely-useable, high-quality tissue maps. Explain the overall strategy for achieving the goals and objectives of the Center and how the different components of the Center will interact to achieve these goals. Specifically, applicants must provide a timeline with details of how the Center will ramp-up data generation and analysis during the funding period. The applicant should also describe metrics associated with evaluating achievement of milestones and what action will be taken, and when, if a milestone is not met or significantly delayed. Applicants should describe how they will prioritize their activities to ensure that the goals of the below. HuBMAP Program will be achieved. Milestones may be revised at the time of the award and yearly as described in the terms and conditions of a Cooperative Agreement
Letters of Support: Provide any letters of support, as appropriate. Include any letters of support for the proposed Center by appropriate institutional officials. Letters should address the commitment of the parent organization, or any of its partners, to the Center and its goals. The parent institution is expected to recognize the Center as a formal organizational component and provide documented evidence of space dedicated to the needs of the Center, protected time to devote to Center activities, staff recruitment, dedicated equipment, or other financial support for the proposed Center. The parent institution should provide assurance of its commitment to continuing support of the Center in the event of a change in directorship and a well-defined plan for this eventuality should be in place. Both the institution and pertinent departments must show a strong commitment to supporting the Center.
If collaborative linkages are being developed between the Center and other local NIH funded centers in related areas a letter of agreement from the collaborating Center PD(s)/PI(s) should be included. Do not provide letters of support from individuals who will not be involved in the Center's research activities.
Resource Sharing Plan: Individuals are required to comply with the instructions for the Resource Sharing Plans as provided in the SF424 (R&R) Application Guide, with the following modification:
Appendix:
Only limited items are allowed in the Appendix. Follow all instructions for the Appendix as described in the SF424 (R&R) Application Guide; any instructions provided here are in addition to the SF424 (R&R) Application Guide instructions.
PHS Human Subjects and Clinical Trials Information (Overall)
When involving human subjects research, clinical research, and/or NIH-defined clinical trials follow all instructions for the PHS Human Subjects and Clinical Trials Information form in the SF424 (R&R) Application Guide, with the following additional instructions:
If you answered Yes to the question Are Human Subjects Involved? on the R&R Other Project Information form, there must be at least one human subjects study record using the Study Record: PHS Human Subjects and Clinical Trials Information form or a Delayed Onset Study record within the application. The study record(s) must be included in the component(s) where the work is being done, unless the same study spans multiple components. To avoid the creation of duplicate study records, a single study record with sufficient information for all involved components must be included in the Overall component when the same study spans multiple components.
Study Record: PHS Human Subjects and Clinical Trials Information
All instructions in the SF424 (R&R) Application Guide must be followed
Delayed Onset Study
Note: Delayed onset does NOT apply to a study that can be described but will not start immediately (i.e., delayed start).
All instructions in the SF424 (R&R) Application Guide must be followed
All instructions in the SF424 (R&R) Application Guide must be followed.
When preparing your application, use Component Type Admin Core.
All instructions in the SF424 (R&R) Application Guide must be followed, with the following additional instructions, as noted.
Complete only the following fields:
Enter Human Embryonic Stem Cells in each relevant component.
Human Subjects: Answer only the Are Human Subjects Involved? and 'Is the Project Exempt from Federal regulations? questions.
Vertebrate Animals: Answer only the Are Vertebrate Animals Used? question.
Project Narrative: Do not complete. Note: ASSIST screens will show an asterisk for this attachment indicating it is required. However, eRA systems only enforce this requirement in the Overall component and applications will not receive an error if omitted in other components.
List all performance sites that apply to the specific component.
Note: The Project Performance Site form allows up to 300 sites, prior to using additional attachment for additional entries.
Budget forms appropriate for the specific component will be included in the application package.
Collaboration: Include funds equating to approximately 20% of the total requested budget for coordination and collaborative activities within the Consortium. These activities will be refined post award. These funds will be restricted and require NIH prior approval for use. A prior approval request will be required to re-allocate these funds to other activities
Note: The R&R Budget form included in many of the component types allows for up to 100 Senior/Key Persons in section A and 100 Equipment Items in section C prior to using attachments for additional entries. All other SF424 (R&R) instructions apply.
Specific Aims: State the specific aims for the Coordination Core and provide a rationale and description of how each aim enhances the operation of the Center and its value to the HuBMAP Consortium.
Research Strategy: In lieu of the standard Research Strategy sub-sections (Significance, Innovation, Approach), use the sub-sections defined below to explain how the Coordination Core will effectively administrate and coordinate the Center's activities:
If external Advisor/Consultants are needed, describe their qualifications and function. Do NOT provide names or biosketches for Advisors/Consultants.
Letters of Support: Include any relevant letters of support, as needed. Do not provide letters of support from individuals who will not be involved in the Center's research activities.
Resource Sharing Plan: Individuals are required to comply with the instructions for the Resource Sharing Plans as provided in the SF424 (R&R) Application Guide, Resource Sharing Plans should only be included in the Overall component.
Appendix:
Only limited items are allowed in the Appendix.Follow all instructions for the Appendix as described in the SF424 (R&R) Application Guide; any instructions provided here are in addition to the SF424 (R&R) Application Guide instructions.
When involving human subjects research, clinical research, and/or NIH-defined clinical trials follow all instructions for the PHS Human Subjects and Clinical Trials Information form in the SF424 (R&R) Application Guide, with the following additional instructions:
If you answered Yes to the question Are Human Subjects Involved? on the R&R Other Project Information form, you must include at least one human subjects study record using the Study Record: PHS Human Subjects and Clinical Trials Information form or a Delayed Onset Study record.
Study Record: PHS Human Subjects and Clinical Trials Information
All instructions in the SF424 (R&R) Application Guide must be followed
Delayed Onset Study
Note: Delayed onset does NOT apply to a study that can be described but will not start immediately (i.e., delayed start).All instructions in the SF424 (R&R) Application Guide must be followed
When preparing your application in ASSIST, use Component Type Core.
All instructions in the SF424 (R&R) Application Guide must be followed, with the following additional instructions, as noted.
Complete only the following fields:
Enter Human Embryonic Stem Cells in each relevant component.
Human Subjects: Answer only the Are Human Subjects Involved? and 'Is the Project Exempt from Federal regulations? questions.
Vertebrate Animals: Answer only the Are Vertebrate Animals Used? question.
Project Narrative: Do not complete. Note: ASSIST screens will show an asterisk for this attachment indicating it is required. However, eRA systems only enforce this requirement in the Overall component and applications will not receive an error if omitted in other components
List all performance sites that apply to the specific component.
Note: The Project Performance Site form allows up to 300 sites, prior to using additional attachment for additional entries.
Budget forms appropriate for the specific component will be included in the application package.
Note: The R&R Budget form included in many of the component types allows for up to 100 Senior/Key Persons in section A and 100 Equipment Items in section C prior to using attachments for additional entries. All other SF424 (R&R) instructions apply.
Specific Aims: State the specific aims of the Data Analysis Core describing how the DAC will assemble tissue maps from the OSPs and upload data to the HIVE.
Research Strategy: Applicants should highlight aspects of the proposed activities of the DAC that speak to the significance and innovation of their approaches. In lieu of the standard Research Strategy subsections (Significance, Innovation, and Approach), describe the activities of the Data Analysis Core using the sub-sections listed below. Describe the outputs from the TMC that will be submitted to the HIVE and the process for doing this in collaboration with the CC.
Data Processing: Describe and demonstrate any existing or proposed data processing pipelines to be employed within the Center, specifically with regards to imaging and omics data collection. State how these pipelines might be scaled to meet the demands of increased throughput within the Center. State the degree to which the resulting processed data is interoperable and meets the qualifications for FAIR data sharing standards. If field standard pipelines are not being employed within the Center, provide justification for the use of in-house pipelines and provide examples of downstream analyses utilizing the output of the pipeline (to demonstrate interoperability). Describe a plan for assessing and management data quality including identification of missing or out of range data, calibration drift, or user variability.
Data Analysis: Describe and demonstrate the computational approaches to be employed within the DAC that will result in the generation of multiscale, multiparameter tissue maps from high-content imaging and omics data from the OSPs. As appropriate, describe strategies that will be used to integrate multiscale data from different spatial resolution assays; integrate disparate omics and imaging data types; automate image analysis to extract and annotate features; and systems biology approaches to connect disparate data.
Map Construction: Describe and demonstrate plans to aggregate and integrate data and metadata from the broad range of experimental and computational approaches outlined throughout the application to build 3D tissue maps. As appropriate, describe how anatomical relationships will be maintained with respect to the donor's body, how samples from the same individual or multiple individuals can be analyzed to understand variability, how ontologies, visualization and image analysis tools will be used to interpret that data and build an atlas of different types of maps. Describe plans to develop and/or adapt computational tools for searching, cross-validation, and data visualization. Describe plans for how data analysis and map generation can optimize the data generation pipeline of the OSPs.
Consortium Coordination: Describe plans to work with the HIVE and other TMCs to develop common data formats and interoperable tools and procedures allowing seamless integration and presentation of the maps generated by the Consortium. Include preliminary plans for coordinating data quality across the Consortium. Describe how proposed analysis workflows or pipelines can be shared and harmonized across the Consortium. Demonstrate through evidence of collaboration and/or open source algorithm and computational tool development the flexibility of the DAC to incorporate disparate data types from emerging technologies incorporated after award. Analytical flexibility is an important aspect because the breadth of data types across the Consortium and technologies that may be employed in the future is currently unknown.
Letters of Support: Include any relevant letters of support, as needed. Do not provide letters of support from individuals who will not be involved in the Center's research activities.
Resource Sharing Plan: Individuals are required to comply with the instructions for the Resource Sharing Plans as provided in the SF424 (R&R) Application Guide, Resource Sharing Plans should only be included in the Overall component.
Appendix:
Limited items are allowed in the Appendix. Follow all instructions for the Appendix as described in the SF424 (R&R) Application Guide; any instructions provided here are in addition to the SF424 (R&R) Application Guide instructions.
When involving NIH-defined human subjects research, clinical research, and/or clinical trials follow all instructions for the PHS Human Subjects and Clinical Trials Information form in the SF424 (R&R) Application Guide, with the following additional instructions:
If you answered Yes to the question Are Human Subjects Involved? on the R&R Other Project Information form, you must include at least one human subjects study record using the Study Record: PHS Human Subjects and Clinical Trials Information form or a Delayed Onset Study record.
Study Record: PHS Human Subjects and Clinical Trials Information
All instructions in the SF424 (R&R) Application Guide must be followed
Delayed Onset Study
All instructions in the SF424 (R&R) Application Guide must be followed
When preparing your application in ASSIST, use Component Type Projects.
All instructions in the SF424 (R&R) Application Guide must be followed, with the following additional instructions, as noted.
Complete only the following fields:
Enter Human Embryonic Stem Cells in each relevant component.
Human Subjects: Answer only the Are Human Subjects Involved? and 'Is the Project Exempt from Federal regulations? questions.
Vertebrate Animals: Answer only the Are Vertebrate Animals Used? question.
Project Narrative: Do not complete. Note: ASSIST screens will show an asterisk for this attachment indicating it is required. However, eRA systems only enforce this requirement in the Overall component and applications will not receive an error if omitted in other components
List all performance sites that apply to the specific component.
Note: The Project Performance Site form allows up to 300 sites, prior to using additional attachment for additional entries.
Budget forms appropriate for the specific component will be included in the application package.
Specific Aims: State the specific aims for the Organ Specific Project and provide a rationale and description of how each aim addresses a specific aspect of generating tissue maps of that organ.
Research Strategy: Applicants should highlight aspects of their proposed activities that speak to the significance and innovation of the approach. In lieu of the standard Research Strategy subsections (Significance, Innovation, and Approach), describe the activities of the Organ Specific Project using the sub-sections listed below.
Biospecimen Management: Provide an overview of how the OSP will collect and analyze biospecimens in a manner that reflects the expected tissue diversity in order to build reliable tissue maps. Describe the type, volume, source and sampling approach for human biospecimen collection, including biological, technical and statistical justification. Provide details of the number of samples that can be acquired and processed each year, specifically stating how the accrual rate will contribute to the Interim and Overall Milestones. Provide details about the breadth of informed consent obtained from donors; biospecimens will potentially be analyzed or re-analyzed later in the Program using new and cutting-edge assays and data tools that will be introduced after award so careful attention must be paid to the design of donor consent forms at the time of specimen collection. Consent forms that allow for broad data sharing are strongly encouraged. Describe plans for collection of appropriate clinical and epidemiological data that will best inform construction and future use of the proposed tissue maps. Include details regarding what biospecimens can and will be shared through a Tissue Core along with details of metadata that will be collected, data standards, how information about location and orientation of tissues will be collected and preserved. Applications are encouraged to present preliminary data that demonstrates awareness of how sample quality can be maximized for a variety of downstream assays.
Pre-Analytical Pipeline: Provide a comprehensive roadmap for sample acquisition, processing, and characterization prior to analysis. Describe how the source, orientation and location of biospecimens will be determined and shared, including a plan for interoperability with other TMCs utilizing a common coordinate system. Describe any anatomical or pathological analyses that will be performed to characterize the specimen at the time of collection. Describing any sampling approaches employed. Describe quality control metrics will be developed and/or employed to ensure high sample quality upon collection, after preservation, and upon pre-analytical processing, including parameters that define sample quality and a plan for sharing quality control measures and information with the Consortium. Describe how the tissue will be processed and/or preserved to facilitate analysis, including optimization of pre-analytical processing of tissue for multiple imaging and omics assays.
Characterization Pipeline: Provide a general overview of the assays that will be deployed and the various data types that will be collected to characterize the tissue. Provide a biological justification for data type, sampling approach and data volume to be acquired that is motivated by the maps to be constructed. Benchmark the sensitivity, specificity and reproducibility of the assays to be deployed and any strategies used to calibrate and optimize them. State if technologies proposed within the application can be considered analytically validated. If not, provide plans and timelines for analytical validation. Provide a workflow for data collection that describes how high-content, high-throughput data at a single cell resolution will be collected for comprehensive characterization of each biospecimen. If assays are in different geographical areas, provide a plan for how biospecimens will be divided or transported for analysis. Describe a strategy to monitor and ensure the quality of instrument performance and data generated across the Center. Applications should describe typical error rates for the proposed assays and steps for data quality management.
Scaling and Standardizing the Pipeline: Describe plans for how the data generation pipeline will be scaled up during the project, including expectations for different datasets to be generated such as preliminary data, calibration data, validation data, and production data. Provide an overview for how the proposed pipeline may be harmonized with those developed by other TMCs. Describe plans for scaling the pipeline including how emerging technologies may be incorporated into the pipeline, optimization of existing assays to enhance throughput or building additional analytical capacity.
Letters of Support: Include any relevant letters of support, as needed. Do not provide letters of support from individuals who will not be involved in the Center's research activities.
Resource Sharing Plan: Individuals are required to comply with the instructions for the Resource Sharing Plans as provided in the SF424 (R&R) Application Guide, Resource Sharing Plans should only be included in the Overall component.
Appendix:
Limited items are allowed in the Appendix. Follow all instructions for the Appendix as described in the SF424 (R&R) Application Guide; any instructions provided here are in addition to the SF424 (R&R) Application Guide instructions.
When involving NIH-defined human subjects research, clinical research, and/or clinical trials follow all instructions for the PHS Human Subjects and Clinical Trials Information form in the SF424 (R&R) Application Guide, with the following additional instructions:
If you answered Yes to the question Are Human Subjects Involved? on the R&R Other Project Information form, you must include at least one human subjects study record using the Study Record: PHS Human Subjects and Clinical Trials Information form or a Delayed Onset Study record.
Study Record: PHS Human Subjects and Clinical Trials Information
All instructions in the SF424 (R&R) Application Guide must be followed
Delayed Onset Study
All instructions in the SF424 (R&R) Application Guide must be followed
See Part 1. Section III.1 for information regarding the requirement for obtaining a unique entity identifier and for completing and maintaining active registrations in System for Award Management (SAM), NATO Commercial and Government Entity (NCAGE) Code (if applicable), eRA Commons, and Grants.gov.
Part I. Overview Information contains information about Key Dates and times. Applicants are encouraged to submit applications before the due date to ensure they have time to make any application corrections that might be necessary for successful submission. When a submission date falls on a weekend or Federal holiday, the application deadline is automatically extended to the next business day.
Organizations must submit applications to Grants.gov (the online portal to find and apply for grants across all Federal agencies) using ASSIST or other electronic submission systems. Applicants must then complete the submission process by tracking the status of the application in the eRA Commons, NIH’s electronic system for grants administration. NIH and Grants.gov systems check the application against many of the application instructions upon submission. Errors must be corrected and a changed/corrected application must be submitted to Grants.gov on or before the application due date and time. If a Changed/Corrected application is submitted after the deadline, the application will be considered late. Applications that miss the due date and time are subjected to the NIH Policy on Late Application Submission.
Applicants are responsible for viewing their application before the due date in the eRA Commons to ensure accurate and successful submission.
Information on the submission process and a definition of on-time submission are provided in the SF424 (R&R) Application Guide.
This initiative is not subject to intergovernmental review.
All NIH awards are subject to the terms and conditions, cost principles, and other considerations described in the NIH Grants Policy Statement.
Pre-award costs are allowable only as described in the NIH Grants Policy Statement.
Applications must be submitted electronically following the instructions described in the SF424 (R&R) Application Guide. Paper applications will not be accepted.
For information on how your application will be automatically assembled for review and funding consideration after submission go to: http://grants.nih.gov/grants/ElectronicReceipt/files/Electronic_Multi-project_Application_Image_Assembly.pdf.
Applicants must complete all required registrations before the application due date. Section III. Eligibility Information contains information about registration.
For assistance with your electronic application or for more information on the electronic submission process, visit How to Apply Application Guide. If you encounter a system issue beyond your control that threatens your ability to complete the submission process on-time, you must follow the Dealing with System Issues guidance. For assistance with application submission, contact the Application Submission Contacts in Section VII.
Important reminders:
All PD(s)/PI(s) and component Project Leads must include their eRA Commons ID in the Credential field of the Senior/Key Person Profile Component of the SF424(R&R) Application Package. Failure to register in the Commons and to include a valid PD/PI Commons ID in the credential field will prevent the successful submission of an electronic application to NIH.
The applicant organization must ensure that the DUNS number it provides on the application is the same number used in the organization’s profile in the eRA Commons and for the System for Award Management (SAM). Additional information may be found in the SF424 (R&R) Application Guide.
See more tips for avoiding common errors.
Upon receipt, applications will be evaluated for completeness and compliance with application instructions by the Center for Scientific Review and responsiveness by components of participating organizations, NIH. Applications that are incomplete, non-compliant and/or nonresponsive will not be reviewed.
The requests by NIH intramural scientists will be limited to the incremental costs required for participation. As such, these requests will not include any salary and related fringe benefits for career, career conditional or other Federal employees (civilian or uniformed service) with permanent appointments under existing position ceilings or any costs related to administrative or facilities support (equivalent to Facilities and Administrative or F&A costs). These costs may include salary for staff to be specifically hired under a temporary appointment for the project, consultant costs, equipment, supplies, travel, and other items typically listed under Other Expenses. Applicants should indicate the number of person-months devoted to the project, even if no funds are requested for salary and fringe benefits.
If selected, appropriate funding will be provided by the Common Fund through the NIH Intramural Program. NIH intramural scientists will participate in this program as PDs/PIs in accord with the Terms and Conditions provided in this FOA. Intellectual property will be managed in accord with established policy of the NIH in compliance with Executive Order 10096, as amended, 45 CFR Part 7; patent rights for inventions developed in NIH facilities are NIH property unless NIH waives its rights.
Should an extramural application include the collaboration with an intramural scientist, no funds for the support of the intramural scientist may be requested in the application. The intramural scientist may submit a separate request for intramural funding as described above.
Many NIH ICs encourage the use of common data elements (CDEs) in basic, clinical, and applied research, patient registries, and other human subject research to facilitate broader and more effective use of data and advance research across studies. CDEs are data elements that have been identified and defined for use in multiple data sets across different studies. Use of CDEs can facilitate data sharing and standardization to improve data quality and enable data integration from multiple studies and sources, including electronic health records. NIH ICs have identified CDEs for many clinical domains (e.g., neurological disease), types of studies (e.g. genome-wide association studies (GWAS)), types of outcomes (e.g., patient-reported outcomes), and patient registries (e.g., the Global Rare Diseases Patient Registry and Data Repository). NIH has established a Common Data Element (CDE) Resource Portal" (http://cde.nih.gov/) to assist investigators in identifying NIH-supported CDEs when developing protocols, case report forms, and other instruments for data collection. The Portal provides guidance about and access to NIH-supported CDE initiatives and other tools and resources for the appropriate use of CDEs and data standards in NIH-funded research. Investigators are encouraged to consult the Portal and describe in their applications any use they will make of NIH-supported CDEs in their projects
Applicants are required to follow the instructions for post-submission materials, as described in the policy. Any instructions provided here are in addition to the instructions in the policy.
Only the review criteria described below will be considered in the review process. Applications submitted to the NIH in support of the NIH mission are evaluated for scientific and technical merit through the NIH peer review system.
Reviewers will provide an overall impact score to reflect their assessment of the likelihood for the Center to exert a sustained, powerful influence on the research field(s) involved, in consideration of the following review criteria and additional review criteria (as applicable for the Center proposed).
Reviewers will consider each of the review criteria below in the determination of scientific merit, and give a separate score for each. An application does not need to be strong in all categories to be judged likely to have major scientific impact. For example, a Center that by its nature is not innovative may be essential to advance a field.
Does the Center address an important problem or a critical barrier to progress in the field? Is the prior research that serves as the key support for the proposed project rigorous? If the aims of the Center are achieved, how will scientific knowledge, technical capability, and/or clinical practice be improved? How will successful completion of the aims change the concepts, methods, technologies, treatments, services, or preventative interventions that drive this field? Will this Center make a significant contribution to the overall goals and objectives of the Human BioMolecular Atlas Program?
Will the data and knowledge generated by this Center lead to a better understanding of the relationship between tissue organization and function?
Are the PD(s)/PI(s), collaborators, and other researchers well suited to the Center? If Early Stage Investigators or those in the early stages of independent careers, do they have appropriate experience and training? If established, have they demonstrated an ongoing record of accomplishments that have advanced their field(s)? If the project is collaborative or multi-PD/PI, do the investigators have complementary and integrated expertise; are their leadership approach, governance and organizational structure appropriate for the project? Do the Center Director and PD(s)/PI(s) have the appropriate experience in managing complex, multi-site projects involving teams of scientists?
Do the PD(s)/PI(s) and research team have a strong track-record of generating, integrating and analyzing high-quality data as part of a consortium?
Does the research team have a strong expertise across all areas of the data generation pipeline and a clear leadership plan for integrating their expertise to meet the specific aims of the Center?
Does the application challenge and seek to shift current research or clinical practice paradigms by utilizing novel theoretical concepts, approaches or methodologies, instrumentation, or interventions? Are the concepts, approaches or methodologies, instrumentation, or interventions novel to one field of research or novel in a broad sense? Is a refinement, improvement, or new application of theoretical concepts, approaches or methodologies, instrumentation, or interventions proposed? Does the project have an optimal balance in proposing state-of-art, cutting-edge technologies and approaches that are also proven, validated and reliable to meet the high content and high throughput expectations for these Centers?
This FOA is not intended to support the development of new technologies, assays or models. However, because new and more powerful technologies emerge in the field, are roadmap and methods for potentially incorporating them in later years sufficiently described? Is the design of those roadmap and methods creative, innovative and likely to maximize the quality of the data generated? Are the data analysis approaches innovative, state-of-the-art and likely to improve tissue collection strategies, assay choices and sampling approaches?
Are the overall strategy, methodology, and analyses well-reasoned and appropriate to accomplish the specific aims of the Center? Have investigators included plans to address weaknesses in the rigor of prior research that serves as the key support for the proposed project? Have the investigators presented strategies to ensure a robust and unbiased approach, as appropriate for the work proposed? Are potential problems, alternative strategies, and benchmarks for success presented? If the project is in the early stages of development, will the strategy establish feasibility and will particularly risky aspects be managed? Have the investigators presented adequate plans to address relevant biological variables, such as sex, for studies in vertebrate animals or human subjects?
If the Center involves human subjects and/or NIH-defined clinical research, are the plans to address:
1) the protection of human subjects from research risks, and
2) inclusion (or exclusion) of individuals on the basis of sex/gender, race, and ethnicity, as well as the inclusion or exclusion of individuals of all ages (including children and older adults), justified in terms of the scientific goals and research strategy proposed? Has the TMC proposed a pipeline for tissue collection and analysis that minimizes degradation, maximizes the quantity and quality of data generated? Are plans to increase the rigor and reproducibility of the data generation acceptable?
Has the Center proposed a suite of assays and approaches that are appropriate for the choice of organs and tissues to be examined? Are the assays complementary in the data they will generate?
Are the assays optimal and well-designed for spatially mapping human tissue in a high-content, high-throughput manner?
Will the research strategy effectively and efficiently result in tissue maps that comprehensively profile a significant number and diverse range of biomolecules present?
Does the plan provide ample opportunity for collaboration, integration, and interaction within the TMC, with the rest of the HuBMAP Consortium and the wider research community?
Is the timeline proposed for ramping up data production reasonable?
Is there synergy between the organ specific projects? Are there inter-dependencies between the OSPs that would prevent them progressing independently?
Will the scientific environment in which the work will be done contribute to the probability of success? Are the institutional support, equipment and other physical resources available to the investigators adequate for the project proposed? Will the project benefit from unique features of the scientific environment, subject populations, or collaborative arrangements? Are the resources, equipment and infrastructure available and in place (or readily obtainable) to achieve the required output from the screening and analysis pipeline?
Are the instrumentation and computational resources in place (or readily obtainable) and adequate to support the project? Are safeguards in place to protect donor personal identifiable information if relevant?
As applicable for the Center proposed, reviewers will evaluate the following additional items while determining scientific and technical merit, and in providing an overall impact score, but will not give separate scores for these items.
For research that involves human subjects but does not involve one of the categories of research that are exempt under 45 CFR Part 46, the committee will evaluate the justification for involvement of human subjects and the proposed protections from research risk relating to their participation according to the following five review criteria: 1) risk to subjects, 2) adequacy of protection against risks, 3) potential benefits to the subjects and others, 4) importance of the knowledge to be gained, and 5) data and safety monitoring for clinical trials.
For research that involves human subjects and meets the criteria for one or more of the categories of research that are exempt under 45 CFR Part 46, the committee will evaluate: 1) the justification for the exemption, 2) human subjects involvement and characteristics, and 3) sources of materials. For additional information on review of the Human Subjects section, please refer to the Guidelines for the Review of Human Subjects.
When the proposed Center involves human subjects and/or NIH-defined clinical research, the committee will evaluate the proposed plans for the inclusion (or exclusion) of individuals on the basis of sex/gender, race, and ethnicity, as well as the inclusion (or exclusion) of individuals of all ages (including children and older adults) to determine if it is justified in terms of the scientific goals and research strategy proposed. For additional information on review of the Inclusion section, please refer to the Guidelines for the Review of Inclusion in Clinical Research.
The committee will evaluate the involvement of live vertebrate animals as part of the scientific assessment according to the following criteria: (1) description of proposed procedures involving animals, including species, strains, ages, sex, and total number to be used; (2) justifications for the use of animals versus alternative models and for the appropriateness of the species proposed; (3) interventions to minimize discomfort, distress, pain and injury; and (4) justification for euthanasia method if NOT consistent with the AVMA Guidelines for the Euthanasia of Animals. Reviewers will assess the use of chimpanzees as they would any other application proposing the use of vertebrate animals. For additional information on review of the Vertebrate Animals section, please refer to the Worksheet for Review of the Vertebrate Animal Section.
Reviewers will assess whether materials or procedures proposed are potentially hazardous to research personnel and/or the environment, and if needed, determine whether adequate protection is proposed.
Not Applicable
Not Applicable
Not Applicable
As applicable for the Center proposed, reviewers will consider each of the following items, but will not give scores for these items, and should not consider them in providing an overall impact score.
Is the budget allocated to each of the components reasonable to support the proposed activities?
Not Applicable.
Reviewers will assess the information provided in this section of the application, including 1) the Select Agent(s) to be used in the proposed research, 2) the registration status of all entities where Select Agent(s) will be used, 3) the procedures that will be used to monitor possession use and transfer of Select Agent(s), and 4) plans for appropriate biosafety, biocontainment, and security of the Select Agent(s).
Reviewers will comment on whether the following Resource Sharing Plans, or the rationale for not sharing the following types of resources, are reasonable: 1) Data Sharing Plan; 2) Sharing Model Organisms; and 3) Genomic Data Sharing Plan ,4) Plan for Public Access, 5) Plan for Protocol, Tool, and Reagent Sharing, 6) Plan for Sharing Software.
For projects involving key biological and/or chemical resources, reviewers will comment on the brief plans proposed for identifying and ensuring the validity of those resources.
Reviewers will consider whether the budget and the requested period of support are fully justified and reasonable in relation to the proposed research.
Applications will be evaluated for scientific and technical merit by (an) appropriate Scientific Review Group(s), convened by the Center for Scientific Review in accordance with NIH peer review policy and procedures, using the stated review criteria. Assignment to a Scientific Review Group will be shown in the eRA Commons.
As part of the scientific peer review, all applications:
Appeals of initial peer review will not be accepted for applications submitted in response to this FOA.
Applications will be assigned on the basis of established PHS referral guidelines to the appropriate NIH Institute or Center. Applications will compete for available funds with all other recommended applications submitted in response to this FOA. Following initial peer review, recommended applications will receive a second level of review by the appropriate national Advisory Council or Board. The following will be considered in making funding decisions:
After the peer review of the application is completed, the PD/PI will be able to access his or her Summary Statement (written critique) via the eRA Commons. Refer to Part 1 for dates for peer review, advisory council review, and earliest start date.
Information regarding the disposition of applications is available in the NIH Grants Policy Statement.
If the application is under consideration for funding, NIH will request "just-in-time" information from the applicant as described in the NIH Grants Policy Statement.
A formal notification in the form of a Notice of Award (NoA) will be provided to the applicant organization for successful applications. The NoA signed by the grants management officer is the authorizing document and will be sent via email to the grantee’s business official.
Awardees must comply with any funding restrictions described in Section IV.5. Funding Restrictions. Selection of an application for award is not an authorization to begin performance. Any costs incurred before receipt of the NoA are at the recipient's risk. These costs may be reimbursed only to the extent considered allowable pre-award costs.
Any application awarded in response to this FOA will be subject to terms and conditions found on the Award Conditions and Information for NIH Grants website. This includes any recent legislation and policy applicable to awards that is highlighted on this website.
Institutional Review Board or Independent Ethics Committee Approval: Grantee institutions must ensure that protocols are reviewed by their IRB or IEC. To help ensure the safety of participants enrolled in NIH-funded studies, the awardee must provide NIH copies of documents related to all major changes in the status of ongoing protocols.
Awardee-selected projects that involve studies involving greater than minimal risk to human subjects} require prior approval by NIH prior to initiation.
All NIH grant and cooperative agreement awards include the NIH Grants Policy Statement as part of the NoA. For these terms of award, see the NIH Grants Policy Statement Part II: Terms and Conditions of NIH Grant Awards, Subpart A: General and Part II: Terms and Conditions of NIH Grant Awards, Subpart B: Terms and Conditions for Specific Types of Grants, Grantees, and Activities. More information is provided at Award Conditions and Information for NIH Grants.
Recipients of federal financial assistance (FFA) from HHS must administer their programs in compliance with federal civil rights law. This means that recipients of HHS funds must ensure equal access to their programs without regard to a person’s race, color, national origin, disability, age and, in some circumstances, sex and religion. This includes ensuring your programs are accessible to persons with limited English proficiency. HHS recognizes that research projects are often limited in scope for many reasons that are nondiscriminatory, such as the principal investigator s scientific interest, funding limitations, recruitment requirements, and other considerations. Thus, criteria in research protocols that target or exclude certain populations are warranted where nondiscriminatory justifications establish that such criteria are appropriate with respect to the health or safety of the subjects, the scientific study design, or the purpose of the research.
For additional guidance regarding how the provisions apply to NIH grant programs, please contact the Scientific/Research Contact that is identified in Section VII under Agency Contacts of this FOA. HHS provides general guidance to recipients of FFA on meeting their legal obligation to take reasonable steps to provide meaningful access to their programs by persons with limited English proficiency. Please see https://www.hhs.gov/civil-rights/for-individuals/special-topics/limited-english-proficiency/index.html. The HHS Office for Civil Rights also provides guidance on complying with civil rights laws enforced by HHS. Please see https://www.hhs.gov/civil-rights/for-individuals/section-1557/index.html; and https://www.hhs.gov/civil-rights/for-providers/laws-regulations-guidance/index.html. Recipients of FFA also have specific legal obligations for serving qualified individuals with disabilities. Please see https://www.hhs.gov/civil-rights/for-individuals/disability/index.html. Please contact the HHS Office for Civil Rights for more information about obligations and prohibitions under federal civil rights laws at https://www.hhs.gov/ocr/about-us/contact-us/index.html or call 1-800-368-1019 or TDD 1-800-537-7697. Also note it is an HHS Departmental goal to ensure access to quality, culturally competent care, including long-term services and supports, for vulnerable populations. For further guidance on providing culturally and linguistically appropriate services, recipients should review the National Standards for Culturally and Linguistically Appropriate Services in Health and Health Care at http://minorityhealth.hhs.gov/omh/browse.aspx?lvl=2&lvlid=53.
In accordance with the statutory provisions contained in Section 872 of the Duncan Hunter National Defense Authorization Act of Fiscal Year 2009 (Public Law 110-417), NIH awards will be subject to the Federal Awardee Performance and Integrity Information System (FAPIIS) requirements. FAPIIS requires Federal award making officials to review and consider information about an applicant in the designated integrity and performance system (currently FAPIIS) prior to making an award. An applicant, at its option, may review information in the designated integrity and performance systems accessible through FAPIIS and comment on any information about itself that a Federal agency previously entered and is currently in FAPIIS. The Federal awarding agency will consider any comments by the applicant, in addition to other information in FAPIIS, in making a judgement about the applicant’s integrity, business ethics, and record of performance under Federal awards when completing the review of risk posed by applicants as described in 45 CFR Part 75.205 Federal awarding agency review of risk posed by applicants. This provision will apply to all NIH grants and cooperative agreements except fellowships.
Cooperative Agreement Terms and Conditions of Award
The following special terms of award are in addition to, and not in lieu of, otherwise applicable U.S. Office of Management and Budget (OMB) administrative guidelines, U.S. Department of Health and Human Services (DHHS) grant administration regulations at 45 CFR Part 75, and other HHS, PHS, and NIH grant administration policies.
The administrative and funding instrument used for this program will be the cooperative agreement, an "assistance" mechanism (rather than an "acquisition" mechanism), in which substantial NIH programmatic involvement with the awardees is anticipated during the performance of the activities. Under the cooperative agreement, the NIH purpose is to support and stimulate the recipients' activities by involvement in and otherwise working jointly with the award recipients in a partnership role; it is not to assume direction, prime responsibility, or a dominant role in the activities. Consistent with this concept, the dominant role and prime responsibility resides with the awardees for the project, although specific tasks and activities may be shared among the awardees and the NIH as defined below.
NIH Working Group (NIH WG): Consists of NIH programmatic staff from multiple Institutes and Centers of the NIH as well as the Office of the Director. This group will be primarily responsible for the stewardship of the HuBMAP Program and will participate as non-voting members in the Consortium committees. The HuBMAP WG is led by the HuBMAP Program Manager and co-chaired by the Directors of NIBIB, NHLBI, and NIDDK. It reports to the Directors of the Office of Strategic Coordination/Common Fund and the Division of Program Coordination, Planning, and Strategic Initiatives for final funding decisions.
HuBMAP Program Manager: The HuBMAP Program Manager is an NIH extramural scientist who is responsible for overall coordination of the Consortium and chairs the NIH WG. They will have substantial involvement in assessing progress and making recommendations about future funding. The HuBMAP Program Manager will have substantial scientific programmatic involvement in the direction of all the HuBMAP awards and may consult other NIH and non-NIH experts in making determinations. They will participate as a non-voting member of all Consortium committees and will review and approve Consortium policies. The HuBMAP Program Manager will not co-author publications with project investigators.
HuBMAP Program Coordinator - One or more NIH Program Staff will serve as Program Coordinators. The HuBMAP Coordinator will have substantial programmatic involvement that is above and beyond the normal stewardship role. The Coordinator will provide cooperation or coordination with, or assistance to, awardees in performing project activities. If feasible, the Coordinator will connect awardees with NIH-supported research resources and identify other researchers or resources that may accelerate the project. The Coordinator will also assist with connecting investigators to other federal agencies, similar consortia and related fields of research. The Coordinator will not co-author publications with project investigators.
External Program Consultants (EPCs): As part of the HuBMAP program, NIH staff will engage 5-10 external program consultants (EPCs) not funded as part of the program but with relevant scientific and consortium experience to provide input and advice to the NIH WG. This could include reviewing and evaluating the progress of the entire HuBMAP Program or individual awardees as well as recommending changes in priorities for the HuBMAP Program based on scientific advances within and outside of the Consortium. The EPCs will be senior, scientific experts who are not directly involved in the activities of the HuBMAP Program and who agreement to a confidentiality policy, engaged on an as-needed basis to advise on specific issues. NIH is solely responsible for appointing EPCs for variable durations of service. EPCs are invited to participate in Consortium meetings and Steering Committees calls and the annual investigators meeting. A subset of EPCs may also meet by phone or web at other times of the year, as needed. Annually, the EPCs will provide individual assessments to the NIH of the progress of the Consortium and will present individual expert recommendations regarding any changes in the HuBMAP Program as necessary. The assessments and recommendations will be provided through the NIH WG to the Director of the Office of Strategic Coordination, NIH
HuBMAP Consortium: The HuBMAP Consortium is made up of HuBMAP awardees, the NIH WG and other scientists and groups the SC agrees to include within the Consortium. The Consortium structure is meant to efficiently and effectively guide all the funded projects to meet the overall goals of the HuBMAP Program.
For each individual award, NIH staff has substantial programmatic involvement that is above and beyond the normal stewardship role in awards, as described below:
NIH Program Officer - A NIH Program Officer (PO) is responsible for the normal scientific and programmatic stewardship, including monitoring progress and compliance with general statutory, regulatory, or policy requirements; discussing and approving milestones and significant changes to the project; and technical assistance to correct performance and facilitate interactions. The PO must approve in advance and in writing annual milestones and any significant changes to the award. The PO also has the option to recommend to the HuBMAP Program Manager, following consultation with the Project Scientist(s), ESCs or the NIH WG, restricting an award based on progress towards milestones, to incentivize rapid development and implementation of policies or collaboration between members of the consortium, or generation of data or resources for use by Consortium members or the wider community. NIH also reserves the right to modify the budget or duration of funding or to curtail an award in the event of: (a) substantive changes in the project not approved in advance, (b) use of funds for activities not within the scope of the specific aims, (c) failure to make sufficient progress toward the project milestones, including timely pre-publication deposition of data or reagents in accordance with approved Consortium Policies, (d) failing to comply with the terms and conditions of the award or establish necessary statutory, regulatory, policy approval required for conducting the project, or (e) ethical or conflict of interest issues. The Program Officer will not co-author publications with project investigators.
NIH Project Scientist(s) - One or more NIH Program Staff will serve as Project Scientists (PSs), for each HuBMAP award and, as appropriate, to oversee collaborative projects amongst awardees and/or other Consortium members. The PSs will serve as the scientific representatives of the NIH to the investigators in accordance with policies and procedures of the cooperative agreement mechanism. If there is more than one PS, one of them will be designated as the Lead PS. The PSs will provide substantial NIH scientific programmatic involvement with the awardee that is anticipated during the performance of the activities supported by this Cooperative Agreement, including review of milestones. PSs will work closely with the PD/PI, the Steering Committee, and the PIs of all projects/cores to maximize progress towards the goals of the project and the program.
PD(s)/PI(s) Responsibilities
The PD(s)/PI(s) will have the primary responsibility for:
NIH Staff Involvement
The NIH will designate program staff, including a Program Officer and a Grants Management Specialist to provide stewardship and administrative oversight of the cooperative agreement. The Program Officer and Grants Management Specialist will be named in the Notice of Grant Award. NIH staff may have substantial programmatic involvement that is above and beyond the normal stewardship role in awards, as described below:
Areas of Joint Responsibility
Close interaction among the participating investigators will be required, as well as significant involvement from the NIH during each phase of the program. The awardees, the PSs, and other designated NIH Staff will participate in the annual in-person investigator meeting and scheduled conference calls and share information on data resources, methodologies, analytical tools, as well as data and preliminary results. PDs/PIs, key co-investigators and pre- and post-doctoral trainees, especially those who are members of under-represented minority groups or those from different but related disciplines, are eligible to attend these meetings. EPCs will attend the annual in person meetings. Other government staff may also attend the annual investigators meetings.
The SC will serve as the main scientific body of the Consortium, with the following roles:
It is anticipated that multiple subcommittees may need to be formed to address important topics. Current working groups include:
Dispute Resolution
Any disagreements that may arise in scientific or programmatic matters (within the scope of the award) between award recipients and the NIH may be brought to Dispute Resolution. A Dispute Resolution Panel will be convened. The panel will have three members: a designee of the SC chosen without NIH staff voting, one NIH designee, and a third designee with expertise in the relevant area who is chosen by the other two; in the case of individual disagreement, the first member may be chosen by the individual awardee. This special dispute resolution procedure does not alter the awardee's right to appeal an adverse action that is otherwise appealable in accordance with PHS regulation 42 CFR Part 50, Subpart D and DHHS regulation 45 CFR Part 16.
When multiple years are involved, awardees will be required to submit the Research Performance Progress Report (RPPR) annually and financial statements as required in the NIH Grants Policy Statement.
A final RPPR, invention statement, and the expenditure data portion of the Federal Financial Report are required for closeout of an award, as described in the NIH Grants Policy Statement.
The Federal Funding Accountability and Transparency Act of 2006 (Transparency Act), includes a requirement for awardees of Federal grants to report information about first-tier subawards and executive compensation under Federal assistance awards issued in FY2011 or later. All awardees of applicable NIH grants and cooperative agreements are required to report to the Federal Subaward Reporting System (FSRS) available at www.fsrs.gov on all subawards over $25,000. See the NIH Grants Policy Statement for additional information on this reporting requirement.
In accordance with the regulatory requirements provided at 45 CFR 75.113 and Appendix XII to 45 CFR Part 75, recipients that have currently active Federal grants, cooperative agreements, and procurement contracts from all Federal awarding agencies with a cumulative total value greater than $10,000,000 for any period of time during the period of performance of a Federal award, must report and maintain the currency of information reported in the System for Award Management (SAM) about civil, criminal, and administrative proceedings in connection with the award or performance of a Federal award that reached final disposition within the most recent five-year period. The recipient must also make semiannual disclosures regarding such proceedings. Proceedings information will be made publicly available in the designated integrity and performance system (currently FAPIIS). This is a statutory requirement under section 872 of Public Law 110-417, as amended (41 U.S.C. 2313). As required by section 3010 of Public Law 111-212, all information posted in the designated integrity and performance system on or after April 15, 2011, except past performance reviews required for Federal procurement contracts, will be publicly available. Full reporting requirements and procedures are found in Appendix XII to 45 CFR Part 75 Award Term and Conditions for Recipient Integrity and Performance Matters.
We encourage inquiries concerning this funding opportunity
and welcome the opportunity to answer questions from potential applicants.
eRA Service Desk (Questions regarding ASSIST, eRA Commons, application errors and warnings, documenting system problems that threaten submission by the due date, and post-submission issues)
Finding Help Online: http://grants.nih.gov/support/ (preferred
method of contact)
Telephone: 301-402-7469 or 866-504-9552 (Toll Free)
General Grants Information
(Questions regarding application instructions, application processes, and NIH
grant resources)
Email: [email protected] (preferred
method of contact)
Telephone: 301-945-7573
Grants.gov Customer Support (Questions regarding Grants.gov
registration and Workspace)
Contact Center Telephone: 800-518-4726
Email: [email protected]
Zorina Galis, Ph.D.
National Heart, Lung and Blood Institute (NHLBI)
Telephone: 301-435-0560
Email: [email protected]
David Balasundaram, Ph.D.
Center for Scientific Review (CSR)
Telephone: 301-435-1022
Email: [email protected]
Tracee Foster
National Heart, Lung and Blood Institute (NHLBI)
Telephone: 301-827-8030
Email: [email protected]
Recently issued trans-NIH policy notices may affect your application submission. A full list of policy notices published by NIH is provided in the NIH Guide for Grants and Contracts. All awards are subject to the terms and conditions, cost principles, and other considerations described in the NIH Grants Policy Statement.
Awards are made under the authorization of Sections 301 and 405 of the Public Health Service Act as amended (42 USC 241 and 284) and under Federal Regulations 42 CFR Part 52 and 45 CFR Part 75.