In Vivo Predictive Dissolution (IPD) and Biopharmaceutical Modeling and Simulation: Future Use of Modern Approaches and Methodologies in a Regulatory Context

Overview

Journal Mol Pharm

Publisher American Chemical Society

Specialty Pharmacology

Date 2017 Feb 15

PMID 28195732

Citations 19

Authors

H Lennernas

A Lindahl

A Van Peer

C Ollier

T Flanagan

R Lionberger

A Nordmark

S Yamashita

L Yu

G L Amidon

V Fischer

E Sjogren

P Zane

M McAllister

B Abrahamsson

Affiliations

Soon will be listed here.

Abstract

The overall objective of OrBiTo, a project within Innovative Medicines Initiative (IMI), is to streamline and optimize the development of orally administered drug products through the creation and efficient application of biopharmaceutics tools. This toolkit will include both experimental and computational models developed on improved understanding of the highly dynamic gastrointestinal (GI) physiology relevant to the GI absorption of drug products in both fasted and fed states. A part of the annual OrBiTo meeting in 2015 was dedicated to the presentation of the most recent progress in the development of the regulatory use of PBPK in silico modeling, in vivo predictive dissolution (IPD) tests, and their application to biowaivers. There are still several areas for improvement of in vitro dissolution testing by means of generating results relevant for the intraluminal conditions in the GI tract. The major opportunity is probably in combining IPD testing and physiologically based in silico models where the in vitro data provide input to the absorption predictions. The OrBiTo project and other current research projects include definition of test media representative for the more distal parts of the GI tract, models capturing supersaturation and precipitation phenomena, and influence of motility waves on shear and other forces of hydrodynamic origin, addressing the interindividual variability in composition and characteristics of GI fluids, food effects, definition of biorelevant buffer systems, and intestinal water volumes. In conclusion, there is currently a mismatch between the extensive industrial usage of modern in vivo predictive tools and very limited inclusion of such data in regulatory files. However, there is a great interest among all stakeholders to introduce recent progresses in prediction of in vivo GI drug absorption into regulatory context.

Citing Articles

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Bi F, Yuan T, Zhang B, Li J, Lin Y, Yang J AAPS PharmSciTech. 2024; 26(1):13.

PMID: 39690309 DOI: 10.1208/s12249-024-03006-2.

Mechanistic Modeling of In Vitro Biopharmaceutic Data for a Weak Acid Drug: A Pathway Towards Deriving Fundamental Parameters for Physiologically Based Biopharmaceutic Modeling.

Kowthavarapu V, Charbe N, Gupta C, Iakovleva T, Stillhart C, Parrott N AAPS J. 2024; 26(3):44.

PMID: 38575716 DOI: 10.1208/s12248-024-00912-y.

Dissolution Profiles of Poorly Soluble Drug Salts in Bicarbonate Buffer.

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Using mechanistic models to support development of complex generic drug products: European Medicines Agency perspective.

Manolis E, Garcia-Arieta A, Lindahl A, Kotzagiorgis E, Limberg J, Holte O CPT Pharmacometrics Syst Pharmacol. 2023; 12(5):556-559.

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Non-Effective Improvement of Absorption for Some Nanoparticle Formulations Explained by Permeability under Non-Sink Conditions.

Sugita K, Takata N, Yonemochi E Pharmaceutics. 2022; 14(4).

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