| Literature DB >> 33058891 |
Neil Parrott1, Sandra Suarez-Sharp2, Filippos Kesisoglou3, Shriram M Pathak4, David Good5, Christian Wagner6, André Dallmann7, James Mullin2, Nikunjkumar Patel8, Arian Emami Riedmaier9, Amitava Mitra10, Kimberly Raines11, James Butler12, Maziar Kakhi13, Min Li11, Yang Zhao11, Eleftheria Tsakalozou14, Talia Flanagan15, Jennifer Dressman16, Xavier Pepin17.
Abstract
This workshop report summarizes the proceedings of Day 2 of a three-day workshop on "Current State and Future Expectations of Translational Modeling Strategies toSupportDrug Product Development, Manufacturing Changes and Controls". From a drug product quality perspective, physiologically based biopharmaceutics modeling (PBBM) is a tool to link variations in the drug product quality attributes to in vivo outcomes enabling the establishment of clinically relevant drug product specifications (CRDPS). Day 2 of the workshop focused on best practices in developing, verifying and validating PBBM. This manuscript gives an overview of podium presentations and summarizes breakout (BO) session discussions related to (1) challenges and opportunities for using PBBM to assess the clinical impact of formulation and manufacturing changes on the in vivo performance of a drug product, (2) best practices to account for parameter uncertainty and variability during model development, (3) best practices in the development, verification and validation of PBBM and (4) opportunities and knowledge gaps related to leveraging PBBM for virtual bioequivalence simulations.Keywords: Biopharmaceutical characterization; Clinical pharmacokinetics; In vitro/In vivo (IVIVC) correlation(s); Oral absorption; Pharmacokinetics; Physiologically based pharmacokinetic (PBPK) modeling; Quality by design (QBD); Taken from the JPS dictionary
Mesh:
Year: 2020 PMID: 33058891 DOI: 10.1016/j.xphs.2020.09.058
Source DB: PubMed Journal: J Pharm Sci ISSN: 0022-3549 Impact factor: 3.534