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Best practices in current models mimicking drug permeability in the gastrointestinal tract - An UNGAP review
Date Issued
2022-03-01
Date Available
2022-06-03T15:57:42Z
Abstract
The absorption of orally administered drug products is a complex, dynamic process, dependant on a range of biopharmaceutical properties; notably the aqueous solubility of a molecule, stability within the gastrointestinal tract (GIT) and permeability. From a regulatory perspective, the concept of high intestinal permeability is intrinsically linked to the fraction of the oral dose absorbed. The relationship between permeability and the extent of absorption means that experimental models of permeability have regularly been used as a surrogate measure to estimate the fraction absorbed. Accurate assessment of a molecule's intestinal permeability is of critical importance during the pharmaceutical development process of oral drug products, and the current review provides a critique of in vivo, in vitro and ex vivo approaches. The usefulness of in silico models to predict drug permeability is also discussed and an overview of solvent systems used in permeability assessments is provided. Studies of drug absorption in humans are an indirect indicator of intestinal permeability, but both in vitro and ex vivo tools provide initial screening approaches and are important tools for assessment of permeability in drug development. Continued refinement of the accuracy of in silico approaches and their validation with human in vivo data will facilitate more efficient characterisation of permeability earlier in the drug development process and will provide useful inputs for integrated, end-to-end absorption modelling.
Sponsorship
European Commission Horizon 2020
Science Foundation Ireland
Other Sponsorship
CÚRAM Centre for Medical Devices
AMBER Centre for Advanced Materials and
BioEngineering Research
Type of Material
Journal Article
Publisher
Elsevier
Journal
European Journal of Pharmaceutical Sciences
Volume
170
Start Page
1
End Page
35
Copyright (Published Version)
2021 The Authors
Language
English
Status of Item
Peer reviewed
ISSN
0928-0987
This item is made available under a Creative Commons License
File(s)
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Name
O'Shea et al Elsevier Open Access.pdf
Size
6.3 MB
Format
Adobe PDF
Checksum (MD5)
858996a838764e3822d89651b0ed55a6
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