This grant aims to develop regulatory standards and guidance for the industry in characterizing critical quality attributes of semisolid topical drug products. The project involves creating a classification system for different types of semisolid dosage forms, identifying quality attributes, and understanding potential failure modes. By studying various classes of semisolid dosage forms, the research will determine critical quality attributes impacting product performance. The ultimate goal is to improve the characterization of semisolid drug products through molecular and macromolecular level analysis, leading to enhanced regulatory standards and safer drug products for the public.
Opportunity ID: 253188
General Information
| Document Type: | Grants Notice |
| Funding Opportunity Number: | RFA-FD-14-010 |
| Funding Opportunity Title: | Characterization of Critical Quality Attributes for Semisolid Topical Drug Products |
| Opportunity Category: | Discretionary |
| Opportunity Category Explanation: | – |
| Funding Instrument Type: | Cooperative Agreement |
| Category of Funding Activity: | Health Science and Technology and other Research and Development |
| Category Explanation: | – |
| Expected Number of Awards: | 5 |
| Assistance Listings: | 93.103 — Food and Drug Administration_Research |
| Cost Sharing or Matching Requirement: | No |
| Version: | Synopsis 3 |
| Posted Date: | Mar 30, 2014 |
| Last Updated Date: | Jun 02, 2014 |
| Original Closing Date for Applications: | Jun 02, 2014 |
| Current Closing Date for Applications: | Jun 09, 2014 A Grace period has been provided through June 9, 2014 for the University of Cincinati due to Grants.gov technical issues resulting in need to install a patch to enable applications submitted through the Coeus interface. |
| Archive Date: | Jul 02, 2014 |
| Estimated Total Program Funding: | $1,250,000 |
| Award Ceiling: | $250,000 |
| Award Floor: | $150,000 |
Eligibility
| Eligible Applicants: | Independent school districts Others (see text field entitled “Additional Information on Eligibility” for clarification) Native American tribal governments (Federally recognized) Public housing authorities/Indian housing authorities County governments Nonprofits that do not have a 501(c)(3) status with the IRS, other than institutions of higher education Native American tribal organizations (other than Federally recognized tribal governments) State governments Small businesses Special district governments For profit organizations other than small businesses Nonprofits having a 501(c)(3) status with the IRS, other than institutions of higher education Private institutions of higher education Public and State controlled institutions of higher education |
| Additional Information on Eligibility: | Foreign Instituttions |
Additional Information
| Agency Name: | Food and Drug Administration |
| Description: | It can be challenging to evaluate whether a proposed semisolid drug product will be suitable for its intended purpose (i.e. complex product quality assessment). Depending upon formulation and manufacturing processes, even products that are Q1/Q2 equivalent could theoretically have Q3 differences in their arrangement of matter that may have the potential to impact dosage form performance. Furthermore, it can be challenging to evaluate potential failure modes for semisolid drug products, because of the wide variety of complex microstructures that can exist within dosage forms that are non-specifically termed creams, lotions, gels, ointments, etc. To address these regulatory science challenges, and to advance FDAs mission to make safe and effective drug products available to the American public, it is essential to keep pace with current technologies that can better characterize semisolid dosage forms, to help identify potential risk factors and failure modes in the proposed drug product, and to facilitate an efficient, relevant and comprehensive Q1/Q2/Q3 comparison of a proposed generic drug product with the RLD. OBLECTIVE: The objective of this work is to support the development of regulatory standards and guidance’s for industry regarding the development of semisolid topical drug products, based upon well-defined critical quality and performance attributes that best characterize these products. DETAILED DESCRIPTION: A preliminary classification system will be developed to comprehensively inventory the various types of semisolid dosage forms relevant to topical drug products, differentiated based upon their components and anticipated microstructures (e.g. single vs. multi-phase gels, oleaginous suspensions, pluronic lecithin organogels, polyethylene glycol or petrolatum-based ointments, oil-in-water or water-in-oil creams, lotions, pastes, etc., each which may have fully or partially dissolved active pharmaceutical ingredient(s) in one or more phases). A theoretical framework for all potential failure modes for each class of semisolid dosage form will be constructed, and since the product container closure system could be associated with a failure mode, it will be considered as well. A comprehensive set of quality attributes will be identified for each class, which may include such physical/chemical attributes as opacity, smoothness, odor, color, consistency, water content, osmolality, pH, etc. However, while it is of interest to monitor all product quality attributes, not all measurable attributes may be critical to product performance or patient acceptability.This project will ultimately help to define critical quality and performance attributes that best characterize topical semisolid drug products. At the molecular level, critical quality (Q1, Q2 and particularly Q3) attributes may potentially encompass not only the components, but also the relative proportions and form of the phase state(s) in the semisolid, globule size and distribution, particle size and distribution of the drug substance(s) within the phases of the dosage form, polymorphic forms of the drug substance, and other potentially critical characteristics as relevant. At the macromolecular level, these Q3 attributes may potentially encompass qualities such as rheology, density, homogeneity, and other physical properties. An essential component of this research would be to identify potential failure modes for different topical semisolid drug products, associate those with variations in critical quality attributes (CQAs) and characterize the formulation, manufacturing or stability-related variables that can influence the CQAs and impact a failure mode (e.g. cream homogenization speed may influence globule size which may impact therapeutic performance).Different classes of semisolid dosage forms will be studied systematically, using formulation or manufacturing alterations to vary different quality attributes, and then using performance tests to identify those attributes that are CQAs. Tests of product performance to evaluate the criticality of quality attributes may be performed with appropriately discriminating in vitro release test (IVRT) methods as described in USP <1724>, or in certain cases with in vitro permeation tests (IVPT) using human skin, or by other methodologies capable of evaluating relative bioavailability. STUDY PHASES: This project will have several phases as noted below:1. Comprehensive description of all potentially measurable physical/chemical qualities of semisolid dosage forms comprised of different components and with different anticipated microstructures and potential failure modes.2. Identification and/or development of appropriate methodologies for measuring each of the quality attributes described for each class of semisolid dosage form.3. Characterization of formulation/manufacturing variables that impact these quality attributes in each class of semisolid dosage form, and 4. Utilization of in vitro and/or in vivo measures of product performance to identify those quality attributes that may be critical to therapeutic performance, and which may be associated with a failure mode for a drug product. |
| Link to Additional Information: | NIH Guide for Grants and Contracts |
| Grantor Contact Information: | If you have difficulty accessing the full announcement electronically, please contact:
Gladys Melendez-Bohler
Grants Management Specialist Phone 301-827-7175 Email:gladys.bohler@fda.hhs.gov |
Version History
| Version | Modification Description | Updated Date |
|---|---|---|
| A Grace period has been provided through June 9, 2014 for the University of Cincinati due to Grants.gov technical issues resulting in need to install a patch to enable applications submitted through the Coeus interface. | Jun 02, 2014 | |
| Edited Eligible recipients. | Jun 02, 2014 | |
| Apr 01, 2014 |
DISPLAYING: Synopsis 3
General Information
| Document Type: | Grants Notice |
| Funding Opportunity Number: | RFA-FD-14-010 |
| Funding Opportunity Title: | Characterization of Critical Quality Attributes for Semisolid Topical Drug Products |
| Opportunity Category: | Discretionary |
| Opportunity Category Explanation: | – |
| Funding Instrument Type: | Cooperative Agreement |
| Category of Funding Activity: | Health Science and Technology and other Research and Development |
| Category Explanation: | – |
| Expected Number of Awards: | 5 |
| Assistance Listings: | 93.103 — Food and Drug Administration_Research |
| Cost Sharing or Matching Requirement: | No |
| Version: | Synopsis 3 |
| Posted Date: | Mar 30, 2014 |
| Last Updated Date: | Jun 02, 2014 |
| Original Closing Date for Applications: | Jun 02, 2014 |
| Current Closing Date for Applications: | Jun 09, 2014 A Grace period has been provided through June 9, 2014 for the University of Cincinati due to Grants.gov technical issues resulting in need to install a patch to enable applications submitted through the Coeus interface. |
| Archive Date: | Jul 02, 2014 |
| Estimated Total Program Funding: | $1,250,000 |
| Award Ceiling: | $250,000 |
| Award Floor: | $150,000 |
Eligibility
| Eligible Applicants: | Independent school districts Others (see text field entitled “Additional Information on Eligibility” for clarification) Native American tribal governments (Federally recognized) Public housing authorities/Indian housing authorities County governments Nonprofits that do not have a 501(c)(3) status with the IRS, other than institutions of higher education Native American tribal organizations (other than Federally recognized tribal governments) State governments Small businesses Special district governments For profit organizations other than small businesses Nonprofits having a 501(c)(3) status with the IRS, other than institutions of higher education Private institutions of higher education Public and State controlled institutions of higher education |
| Additional Information on Eligibility: | Foreign Instituttions |
Additional Information
| Agency Name: | Food and Drug Administration |
| Description: | It can be challenging to evaluate whether a proposed semisolid drug product will be suitable for its intended purpose (i.e. complex product quality assessment). Depending upon formulation and manufacturing processes, even products that are Q1/Q2 equivalent could theoretically have Q3 differences in their arrangement of matter that may have the potential to impact dosage form performance. Furthermore, it can be challenging to evaluate potential failure modes for semisolid drug products, because of the wide variety of complex microstructures that can exist within dosage forms that are non-specifically termed creams, lotions, gels, ointments, etc. To address these regulatory science challenges, and to advance FDAs mission to make safe and effective drug products available to the American public, it is essential to keep pace with current technologies that can better characterize semisolid dosage forms, to help identify potential risk factors and failure modes in the proposed drug product, and to facilitate an efficient, relevant and comprehensive Q1/Q2/Q3 comparison of a proposed generic drug product with the RLD. OBLECTIVE: The objective of this work is to support the development of regulatory standards and guidance’s for industry regarding the development of semisolid topical drug products, based upon well-defined critical quality and performance attributes that best characterize these products. DETAILED DESCRIPTION: A preliminary classification system will be developed to comprehensively inventory the various types of semisolid dosage forms relevant to topical drug products, differentiated based upon their components and anticipated microstructures (e.g. single vs. multi-phase gels, oleaginous suspensions, pluronic lecithin organogels, polyethylene glycol or petrolatum-based ointments, oil-in-water or water-in-oil creams, lotions, pastes, etc., each which may have fully or partially dissolved active pharmaceutical ingredient(s) in one or more phases). A theoretical framework for all potential failure modes for each class of semisolid dosage form will be constructed, and since the product container closure system could be associated with a failure mode, it will be considered as well. A comprehensive set of quality attributes will be identified for each class, which may include such physical/chemical attributes as opacity, smoothness, odor, color, consistency, water content, osmolality, pH, etc. However, while it is of interest to monitor all product quality attributes, not all measurable attributes may be critical to product performance or patient acceptability.This project will ultimately help to define critical quality and performance attributes that best characterize topical semisolid drug products. At the molecular level, critical quality (Q1, Q2 and particularly Q3) attributes may potentially encompass not only the components, but also the relative proportions and form of the phase state(s) in the semisolid, globule size and distribution, particle size and distribution of the drug substance(s) within the phases of the dosage form, polymorphic forms of the drug substance, and other potentially critical characteristics as relevant. At the macromolecular level, these Q3 attributes may potentially encompass qualities such as rheology, density, homogeneity, and other physical properties. An essential component of this research would be to identify potential failure modes for different topical semisolid drug products, associate those with variations in critical quality attributes (CQAs) and characterize the formulation, manufacturing or stability-related variables that can influence the CQAs and impact a failure mode (e.g. cream homogenization speed may influence globule size which may impact therapeutic performance).Different classes of semisolid dosage forms will be studied systematically, using formulation or manufacturing alterations to vary different quality attributes, and then using performance tests to identify those attributes that are CQAs. Tests of product performance to evaluate the criticality of quality attributes may be performed with appropriately discriminating in vitro release test (IVRT) methods as described in USP <1724>, or in certain cases with in vitro permeation tests (IVPT) using human skin, or by other methodologies capable of evaluating relative bioavailability. STUDY PHASES: This project will have several phases as noted below:1. Comprehensive description of all potentially measurable physical/chemical qualities of semisolid dosage forms comprised of different components and with different anticipated microstructures and potential failure modes.2. Identification and/or development of appropriate methodologies for measuring each of the quality attributes described for each class of semisolid dosage form.3. Characterization of formulation/manufacturing variables that impact these quality attributes in each class of semisolid dosage form, and 4. Utilization of in vitro and/or in vivo measures of product performance to identify those quality attributes that may be critical to therapeutic performance, and which may be associated with a failure mode for a drug product. |
| Link to Additional Information: | NIH Guide for Grants and Contracts |
| Grantor Contact Information: | If you have difficulty accessing the full announcement electronically, please contact:
Gladys Melendez-Bohler
Grants Management Specialist Phone 301-827-7175 Email:gladys.bohler@fda.hhs.gov |
DISPLAYING: Synopsis 2
General Information
| Document Type: | Grants Notice |
| Funding Opportunity Number: | RFA-FD-14-010 |
| Funding Opportunity Title: | Characterization of Critical Quality Attributes for Semisolid Topical Drug Products |
| Opportunity Category: | Discretionary |
| Opportunity Category Explanation: | – |
| Funding Instrument Type: | Cooperative Agreement |
| Category of Funding Activity: | Health Science and Technology and other Research and Development |
| Category Explanation: | – |
| Expected Number of Awards: | 5 |
| Assistance Listings: | 93.103 — Food and Drug Administration_Research |
| Cost Sharing or Matching Requirement: | No |
| Version: | Synopsis 2 |
| Posted Date: | Jun 02, 2014 |
| Last Updated Date: | – |
| Original Closing Date for Applications: | – |
| Current Closing Date for Applications: | Jun 02, 2014 |
| Archive Date: | Jul 02, 2014 |
| Estimated Total Program Funding: | $1,250,000 |
| Award Ceiling: | $250,000 |
| Award Floor: | $150,000 |
Eligibility
| Eligible Applicants: | Independent school districts Nonprofits having a 501(c)(3) status with the IRS, other than institutions of higher education County governments Public and State controlled institutions of higher education Public housing authorities/Indian housing authorities Private institutions of higher education Native American tribal governments (Federally recognized) State governments Native American tribal organizations (other than Federally recognized tribal governments) Nonprofits that do not have a 501(c)(3) status with the IRS, other than institutions of higher education Special district governments Others (see text field entitled “Additional Information on Eligibility” for clarification) For profit organizations other than small businesses Small businesses |
| Additional Information on Eligibility: | Foreign Instituttions |
Additional Information
| Agency Name: | Food and Drug Administration |
| Description: | It can be challenging to evaluate whether a proposed semisolid drug product will be suitable for its intended purpose (i.e. complex product quality assessment). Depending upon formulation and manufacturing processes, even products that are Q1/Q2 equivalent could theoretically have Q3 differences in their arrangement of matter that may have the potential to impact dosage form performance. Furthermore, it can be challenging to evaluate potential failure modes for semisolid drug products, because of the wide variety of complex microstructures that can exist within dosage forms that are non-specifically termed creams, lotions, gels, ointments, etc. To address these regulatory science challenges, and to advance FDAs mission to make safe and effective drug products available to the American public, it is essential to keep pace with current technologies that can better characterize semisolid dosage forms, to help identify potential risk factors and failure modes in the proposed drug product, and to facilitate an efficient, relevant and comprehensive Q1/Q2/Q3 comparison of a proposed generic drug product with the RLD. OBLECTIVE: The objective of this work is to support the development of regulatory standards and guidance’s for industry regarding the development of semisolid topical drug products, based upon well-defined critical quality and performance attributes that best characterize these products. DETAILED DESCRIPTION: A preliminary classification system will be developed to comprehensively inventory the various types of semisolid dosage forms relevant to topical drug products, differentiated based upon their components and anticipated microstructures (e.g. single vs. multi-phase gels, oleaginous suspensions, pluronic lecithin organogels, polyethylene glycol or petrolatum-based ointments, oil-in-water or water-in-oil creams, lotions, pastes, etc., each which may have fully or partially dissolved active pharmaceutical ingredient(s) in one or more phases). A theoretical framework for all potential failure modes for each class of semisolid dosage form will be constructed, and since the product container closure system could be associated with a failure mode, it will be considered as well. A comprehensive set of quality attributes will be identified for each class, which may include such physical/chemical attributes as opacity, smoothness, odor, color, consistency, water content, osmolality, pH, etc. However, while it is of interest to monitor all product quality attributes, not all measurable attributes may be critical to product performance or patient acceptability.This project will ultimately help to define critical quality and performance attributes that best characterize topical semisolid drug products. At the molecular level, critical quality (Q1, Q2 and particularly Q3) attributes may potentially encompass not only the components, but also the relative proportions and form of the phase state(s) in the semisolid, globule size and distribution, particle size and distribution of the drug substance(s) within the phases of the dosage form, polymorphic forms of the drug substance, and other potentially critical characteristics as relevant. At the macromolecular level, these Q3 attributes may potentially encompass qualities such as rheology, density, homogeneity, and other physical properties. An essential component of this research would be to identify potential failure modes for different topical semisolid drug products, associate those with variations in critical quality attributes (CQAs) and characterize the formulation, manufacturing or stability-related variables that can influence the CQAs and impact a failure mode (e.g. cream homogenization speed may influence globule size which may impact therapeutic performance).Different classes of semisolid dosage forms will be studied systematically, using formulation or manufacturing alterations to vary different quality attributes, and then using performance tests to identify those attributes that are CQAs. Tests of product performance to evaluate the criticality of quality attributes may be performed with appropriately discriminating in vitro release test (IVRT) methods as described in USP <1724>, or in certain cases with in vitro permeation tests (IVPT) using human skin, or by other methodologies capable of evaluating relative bioavailability. STUDY PHASES: This project will have several phases as noted below:1. Comprehensive description of all potentially measurable physical/chemical qualities of semisolid dosage forms comprised of different components and with different anticipated microstructures and potential failure modes.2. Identification and/or development of appropriate methodologies for measuring each of the quality attributes described for each class of semisolid dosage form.3. Characterization of formulation/manufacturing variables that impact these quality attributes in each class of semisolid dosage form, and 4. Utilization of in vitro and/or in vivo measures of product performance to identify those quality attributes that may be critical to therapeutic performance, and which may be associated with a failure mode for a drug product. |
| Link to Additional Information: | NIH Guide for Grants and Contracts |
| Grantor Contact Information: | If you have difficulty accessing the full announcement electronically, please contact:
Gladys Melendez-Bohler
Grants Management Specialist Phone 301-827-7175 Email:gladys.bohler@fda.hhs.gov |
DISPLAYING: Synopsis 1
General Information
| Document Type: | Grants Notice |
| Funding Opportunity Number: | RFA-FD-14-010 |
| Funding Opportunity Title: | Characterization of Critical Quality Attributes for Semisolid Topical Drug Products |
| Opportunity Category: | Discretionary |
| Opportunity Category Explanation: | – |
| Funding Instrument Type: | Cooperative Agreement |
| Category of Funding Activity: | Health Science and Technology and other Research and Development |
| Category Explanation: | – |
| Expected Number of Awards: | 5 |
| Assistance Listings: | 93.103 — Food and Drug Administration_Research |
| Cost Sharing or Matching Requirement: | No |
| Version: | Synopsis 1 |
| Posted Date: | Apr 01, 2014 |
| Last Updated Date: | – |
| Original Closing Date for Applications: | – |
| Current Closing Date for Applications: | Jun 02, 2014 |
| Archive Date: | Jul 02, 2014 |
| Estimated Total Program Funding: | $1,250,000 |
| Award Ceiling: | $250,000 |
| Award Floor: | $150,000 |
Eligibility
| Eligible Applicants: | Others (see text field entitled “Additional Information on Eligibility” for clarification) Unrestricted (i.e., open to any type of entity above), subject to any clarification in text field entitled “Additional Information on Eligibility” |
| Additional Information on Eligibility: | Foreign Instituttions |
Additional Information
| Agency Name: | Food and Drug Administration |
| Description: | It can be challenging to evaluate whether a proposed semisolid drug product will be suitable for its intended purpose (i.e. complex product quality assessment). Depending upon formulation and manufacturing processes, even products that are Q1/Q2 equivalent could theoretically have Q3 differences in their arrangement of matter that may have the potential to impact dosage form performance. Furthermore, it can be challenging to evaluate potential failure modes for semisolid drug products, because of the wide variety of complex microstructures that can exist within dosage forms that are non-specifically termed creams, lotions, gels, ointments, etc.
To address these regulatory science challenges, and to advance FDAs mission to make safe and effective drug products available to the American public, it is essential to keep pace with current technologies that can better characterize semisolid dosage forms, to help identify potential risk factors and failure modes in the proposed drug product, and to facilitate an efficient, relevant and comprehensive Q1/Q2/Q3 comparison of a proposed generic drug product with the RLD. OBLECTIVE: The objective of this work is to support the development of regulatory standards and guidance’s for industry regarding the development of semisolid topical drug products, based upon well-defined critical quality and performance attributes that best characterize these products. DETAILED DESCRIPTION: A preliminary classification system will be developed to comprehensively inventory the various types of semisolid dosage forms relevant to topical drug products, differentiated based upon their components and anticipated microstructures (e.g. single vs. multi-phase gels, oleaginous suspensions, pluronic lecithin organogels, polyethylene glycol or petrolatum-based ointments, oil-in-water or water-in-oil creams, lotions, pastes, etc., each which may have fully or partially dissolved active pharmaceutical ingredient(s) in one or more phases). A theoretical framework for all potential failure modes for each class of semisolid dosage form will be constructed, and since the product container closure system could be associated with a failure mode, it will be considered as well. A comprehensive set of quality attributes will be identified for each class, which may include such physical/chemical attributes as opacity, smoothness, odor, color, consistency, water content, osmolality, pH, etc. However, while it is of interest to monitor all product quality attributes, not all measurable attributes may be critical to product performance or patient acceptability. This project will ultimately help to define critical quality and performance attributes that best characterize topical semisolid drug products. At the molecular level, critical quality (Q1, Q2 and particularly Q3) attributes may potentially encompass not only the components, but also the relative proportions and form of the phase state(s) in the semisolid, globule size and distribution, particle size and distribution of the drug substance(s) within the phases of the dosage form, polymorphic forms of the drug substance, and other potentially critical characteristics as relevant. At the macromolecular level, these Q3 attributes may potentially encompass qualities such as rheology, density, homogeneity, and other physical properties. An essential component of this research would be to identify potential failure modes for different topical semisolid drug products, associate those with variations in critical quality attributes (CQAs) and characterize the formulation, manufacturing or stability-related variables that can influence the CQAs and impact a failure mode (e.g. cream homogenization speed may influence globule size which may impact therapeutic performance). Different classes of semisolid dosage forms will be studied systematically, using formulation or manufacturing alterations to vary different quality attributes, and then using performance tests to identify those attributes that are CQAs. Tests of product performance to evaluate the criticality of quality attributes may be performed with appropriately discriminating in vitro release test (IVRT) methods as described in USP <1724>, or in certain cases with in vitro permeation tests (IVPT) using human skin, or by other methodologies capable of evaluating relative bioavailability. STUDY PHASES: This project will have several phases as noted below: 1. Comprehensive description of all potentially measurable physical/chemical qualities of semisolid dosage forms comprised of different components and with different anticipated microstructures and potential failure modes. 2. Identification and/or development of appropriate methodologies for measuring each of the quality attributes described for each class of semisolid dosage form. 3. Characterization of formulation/manufacturing variables that impact these quality attributes in each class of semisolid dosage form, and 4. Utilization of in vitro and/or in vivo measures of product performance to identify those quality attributes that may be critical to therapeutic performance, and which may be associated with a failure mode for a drug product. |
| Link to Additional Information: | NIH Guide for Grants and Contracts |
| Grantor Contact Information: | If you have difficulty accessing the full announcement electronically, please contact:
Gladys Melendez-Bohler
Grants Management Specialist Phone 301-827-7175 Email:gladys.bohler@fda.hhs.gov |
Related Documents
Folder 253188 Full Announcement-2 -> rfa-fd-14-010 characterization of critical quality attributes for semisolid topical drug products (u01).pdf
Folder 253188 Full Announcement-3 -> NOT-FD-14-010 posted.pdf
Packages
| Agency Contact Information: | Gladys Melendez-Bohler Grants Management Specialist Phone 301-827-7175 Email: gladys.bohler@fda.hhs.gov |
| Who Can Apply: | Organization Applicants |
| Assistance Listing Number | Competition ID | Competition Title | Opportunity Package ID | Opening Date | Closing Date | Actions |
|---|---|---|---|---|---|---|
| 93.103 | ADOBE-FORMS-C | RFA-FD-14-010 | PKG00194630 | Apr 07, 2014 | Jun 02, 2014 | View |
Package 1
Mandatory forms
253188 RR_SF424_2_0-2.0.pdf
253188 PHS398_ResearchPlan_2_0-2.0.pdf
253188 PHS398_CoverPageSupplement_2_0-2.0.pdf
253188 RR_Budget_1_3-1.3.pdf
253188 RR_KeyPersonExpanded_2_0-2.0.pdf
253188 RR_OtherProjectInfo_1_3-1.3.pdf
253188 PerformanceSite_2_0-2.0.pdf
Optional forms
253188 PlannedReport-1.0.pdf
253188 PHS398_CumulativeInclusionReport-1.0.pdf
253188 RR_SubawardBudget30_1_3-1.3.pdf
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