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FBO DAILY - FEDBIZOPPS ISSUE OF JUNE 24, 2016 FBO #5327
SOURCES SOUGHT

A -- CRO Support for NCATS Bioanalytical Method Development for Biologics

Notice Date
6/22/2016
 
Notice Type
Sources Sought
 
NAICS
541712 — Research and Development in the Physical, Engineering, and Life Sciences (except Biotechnology)
 
Contracting Office
Department of Health and Human Services, National Institutes of Health, National Institute on Drug Abuse, 6001 Executive Boulevard, Room 3155, MSC 9593, Bethesda, Maryland, 20892, United States
 
ZIP Code
20892
 
Solicitation Number
HHS-NIH-NCATS-SBSS-16-005
 
Archive Date
7/29/2016
 
Point of Contact
Lisa Bielen, Phone: (301)451-7167, Jeff Schmidt, Phone: (301) 402-1488
 
E-Mail Address
lisa.bielen@nih.gov, schmidtjr@mail.nih.gov
(lisa.bielen@nih.gov, schmidtjr@mail.nih.gov)
 
Small Business Set-Aside
N/A
 
Description
This is a Small Business Sources Sought notice. This is NOT a solicitation for proposals, proposal abstracts, or quotations. The purpose of this notice is to obtain information regarding: (1) the availability and capability of qualified small business sources; (2) whether they are small businesses; HUBZone small businesses; service-disabled, veteran-owned small businesses; 8(a) small businesses; veteran-owned small businesses; woman-owned small businesses; or small disadvantaged businesses; and (3) their size classification relative to the North American Industry Classification System (NAICS) code for the proposed acquisition. Your responses to the information requested will assist the Government in determining the appropriate acquisition method, including whether a set-aside is possible. An organization that is not considered a small business under the applicable NAICS code should not submit a response to this notice. Please note that to qualify as an eligible small business for purposes of a small business set-aside, at least 50% of the cost of contract performance incurred for personnel must be expended for employees of the small business awardee (see FAR 52.219-14 Limitations on Subcontracting). Background & Purpose Researchers nationwide and across the globe face common barriers in translational research that can delay the development of new interventions for patients in need. The National Center for Advancing Translational Sciences (NCATS) at the National Institutes of Health (NIH) studies translation on a system-wide level as a scientific and operational problem to accelerate the development of treatments and preventive strategies for a wide range of diseases. Within NCATS, the Division of Pre-Clinical Innovation (DPI) plans, conducts and uses both internal and contract resources to advance collaborative research projects across the pre-clinical phases of the translational science spectrum. Contract research organizations (CROs) provide manufacturing, pharmacology, toxicology, regulatory and clinical operations services to DPI to assist with probe and assay development, lead selection and optimization, and Investigational New Drug (IND)-directed studies. The objectives of the Translational Research in Pharmacokinetics and Drug Metabolism (TRPDM) Program are to study absorption, distribution, metabolism and elimination (ADME) properties of novel therapeutics and to clarify the relationship between drug concentrations and efficacy of toxicity in vivo. In order to determine Pharmacokinetics (PK) of therapeutic biologics, quantitative bioanalytical assays for biologics and anti-drug antibodies are required. These assays will be used to support preclinical and clinical studies conducted under the Therapeutics for Rare and Neglected Diseases (TRND) Program. Note: no human subject testing is to be performed under this contract. Project Requirements Written capability statements should demonstrate your organization's ability and related experience in one or more of the following separate Technical Areas: (1) Reagent Generation, (2) Bioanalytical Method Development for A Novel Biologic Drug and Anti-Drug Antibody (ADA), (3) Bioanalysis of a Novel Biologic Drug and ADA in Biologic Matrices, and (4) Determination of Anti-Drug Neutralizing Antibodies. If your organization has capabilities in one or more of the listed Technical Areas, your response must separately describe the organization's ability and related experience for each separate Technical Area. 1.Reagent Generation (a)Develop polyclonal anti-drug antibodies (ideally with active epitope neutralizing activity). (b)Develop monoclonal anti-drug antibodies (ideally at least one with active epitope neutralizing activity). (c)Characterize the specificity of the antibodies (with respect to their reactivity towards to drug specific active epitope(s)). (d)Produce purified and modified antibod(y/ies) suitable for assay development. (e)Conduct work in accordance with site-specific Standard Operating Procedures (SOP). (f)Maintain batch records and detailed information on procedures used to generate and characterize the reagents. 2.Bioanalytical Method Development for A Novel Biologic Drug (a)Develop a sensitive bioanalytical method for the quantitative analysis of a novel biologic in plasma/serum, tissue homogenates and other biological fluids; In addition, assays for the measurement of ADA will be developed. (b)Utilize bioanalytical methods, including (but not limited to) Enzyme-linked Immunosorbent Assay (ELISA), Electrochemiluminescence (ECL), hybrid LC-MS-ligand binding assay (LBA), other appropriate LBA platform, radioimmunoassay (RIA), LC-MS, or quantitative PCR, could be utilized to achieve the required sensitivity and accuracy. (c)Employ accurate, precise, specific/selective and reproducible methods, with standard curves containing a minimum of six (6) non-zero concentration points. The methods should be verified or validated for appropriate accuracy and precision, specificity and selectivity using low, medium and high concentration Quality Control (QC) samples and shown to be suitable for measurement of a novel biologic in concentration ranges expected to be present in study samples. (d)Determine the stability of a novel biologic in blood/plasma/serum, tissue homogenates or other biologic fluids to guide sample collection process in animal studies or clinic trials. Instructions on precaution or method(s) to prevent degradation of a novel biologic in biologic fluids during sample handling should be provided. 3.Bioanalysis of a Novel Biologic Drug in Biologic Matrices (a)Provide bioanalytical support for drug concentration and ADA measurement for samples collected from animal PK and efficacy studies as well as from human clinical trials. (b)Validate assays for measurement of drug concentrations and anti-drug antibodies in accordance with current regulatory guidelines and expectations. (c)Document any deviation from a validated method. (d)Perform sample reanalysis for samples analyzed in Good Laboratory Practices (GLP) or clinical studies. (e)Create bioanalytical reports for drug concentrations in biologic matrices upon completion of the assay. (f)Validate parameters of Toxicokinetics (TK) in GLP Studies and PK in human clinical trials including (but not limited to) area under the concentration-time curve (AUC), maximum drug concentration (Cmax), time to reach Cmax (Tmax), clearance, half-life (t1/2), volume of distribution, and bioavailability with the appropriate software accepted for the regulatory filing purposes. (g)Document sample receiving conditions, sample ID, sample storage conditions and duration. (h)Maintain all completed study documentation for up to five (5) years including laboratory notebooks, source documents, observations, or notations of activities. 4.Determination of Anti-Drug Neutralizing Antibodies (a)Perform the detection and quantitative measurement on the neutralizing antibodies in human clinical samples using cell based assays. (b)Validate the assay and perform the analysis using the validated assay. (c)Document sample receiving conditions, sample ID, sample storage conditions and duration. (d)Maintain all completed study documentation for up to five (5) years including laboratory notebooks, source documents, observations, or notations of activities. Additional Information Specify whether your organization uses any proprietary technology for any of the activities described for Technical Areas 1, 2, 3, or 4. If so, clarify whether NCATS and NCATS Collaborators will have freedom to use the technology at a third party facility in case the project is later transferred to a third party. In addition, your organization's capability statement should: (1)Indicate how many staff members (e.g. Principal Investigators and Technical Scientists) the small business would be able to dedicate to the program, and which of those would be available in-house; (2)Identify which requirements would be performed in-house versus those that would be performed outside your organization; and (3)Describe your organization's ability to rapidly scale staff capacity up or down to support the anticipated workload. Anticipated Period of Performance The Government anticipates making multiple Indefinite Delivery/Indefinite Quantity (ID/IQ) type contract awards under the future solicitation-each with a five year ordering period. The Government anticipates awards will be made in the fourth quarter of FY2017. Other Important Considerations Data and documentation generated under this program could be used for regulatory filing purposes. When required, data and documents must be prepared in a form acceptable to the Food and Drug Administration (FDA) for inclusion in a Drug Master File (DMF), IND application, or New Drug Application (NDA). To enable Collaborators to retain control of the intellectual property for compounds created through the TRCMC program, the Government has sought a Declaration of Exceptional Circumstances (DEC) to the Federal Acquisition Regulations (FAR) for this program. Required Information All capability statements must provide the following: (1) DUNS number; (2) organization name; (3) organization address; (4) point of contact; (5) point of contact title, address, telephone, and email address; and (6) size and type of business (e.g., 8(a), HUBZone, etc.) pursuant the applicable NAICS code. Submission Instructions and Due Date Written capability statements must be SUBMITTED NO LATER THAN Thursday, July 14, 2016 to the below Contracting Office Address, Attn: Lisa Bielen. Electronic capability statements will be accepted by the primary point of contact. Disclaimer and Important Notes This notice does not obligate the Government to award a contract or otherwise pay for the information provided in response. The Government reserves the right to use information provided by respondents for any purpose deemed necessary and legally appropriate. Any organization responding to this notice should ensure that its response is complete and sufficiently detailed to allow the Government to determine the organization's qualifications to perform the work. Respondents are advised that the Government is under no obligation to acknowledge receipt of the information received or provide feedback to respondents with respect to any information submitted. After a review of the responses received, a pre-solicitation synopsis and solicitation may be published in Federal Business Opportunities. However, responses to this notice will not be considered adequate responses to a solicitation. Confidentiality No proprietary, classified, confidential, or sensitive information should be included in your response. The Government reserves the right to use any non-proprietary technical information in any resultant solicitation(s). Contracting Office Address NINDS R&D Contracts Management Branch NCATS Section 6001 Executive Boulevard Suite 3287, MSC 9531 Bethesda, Maryland 20892-9531* *Use Rockville, MD 20852 for Fed-Ex/USPS/Courier/Hand-Delivery Points of Contact Primary Point of Contact: Lisa Bielen Contracting Officer lisa.bielen@nih.gov Phone: (301) 451-7167 Secondary Point of Contact: Jeffrey Schmidt Contracting Officer schmidtjr@mail.nih.gov Phone: (301) 402-1488
 
Web Link
FBO.gov Permalink
(https://www.fbo.gov/spg/HHS/NIH/NIDA-01/HHS-NIH-NCATS-SBSS-16-005/listing.html)
 
Record
SN04158666-W 20160624/160622234927-ff4d8a6b1aba1ea55ad88744e9c15469 (fbodaily.com)
 
Source
FedBizOpps Link to This Notice
(may not be valid after Archive Date)
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