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Impact of gastrointestinal tract variability on oral drug absorption and pharmacokinetics

Authors :
Zahari Vinarov
Mohammad Abdallah
José A.G. Agundez
K.M. (Karel) Allegaert
Abdul W. Basit
Marlies Braeckmans
Jens Ceulemans
Maura Corsetti
Brendan T. Griffin
M Grimm
Daniel Keszthelyi
Mirko Koziolek
Christine M. Madla
Christophe Matthys
Laura E. McCoubrey
Amitava Mitra
Christos Reppas
Jef Stappaerts
Nele Steenackers
Natalie L. Trevaskis
Tim Vanuytsel
Maria Vertzoni
Werner Weitschies
Clive Wilson
Patrick Augustijns
Zahari Vinarov
Mohammad Abdallah
José A.G. Agundez
K.M. (Karel) Allegaert
Abdul W. Basit
Marlies Braeckmans
Jens Ceulemans
Maura Corsetti
Brendan T. Griffin
M Grimm
Daniel Keszthelyi
Mirko Koziolek
Christine M. Madla
Christophe Matthys
Laura E. McCoubrey
Amitava Mitra
Christos Reppas
Jef Stappaerts
Nele Steenackers
Natalie L. Trevaskis
Tim Vanuytsel
Maria Vertzoni
Werner Weitschies
Clive Wilson
Patrick Augustijns
Publication Year :
2021

Abstract

The absorption of oral drugs is frequently plagued by significant variability with potentially serious therapeutic consequences. The source of variability can be traced back to interindividual variability in physiology, differences in special populations (age- and disease-dependent), drug and formulation properties, or food-drug interactions. Clinical evidence for the impact of some of these factors on drug pharmacokinetic variability is mounting: e.g. gastric pH and emptying time, small intestinal fluid properties, differences in pediatrics and the elderly, and surgical changes in gastrointestinal anatomy. However, the link of colonic factors variability (transit time, fluid composition, microbiome), sex differences (male vs. female) and gut-related diseases (chronic constipation, anorexia and cachexia) to drug absorption variability has not been firmly established yet. At the same time, a way to decrease oral drug pharmacokinetic variability is provided by the pharmaceutical industry: clinical evidence suggests that formulation approaches employed during drug development can decrease the variability in oral exposure

Details

Database :
OAIster
Notes :
European Journal of Pharmaceutical Sciences vol. 162
Publication Type :
Electronic Resource
Accession number :
edsoai.on1273464757
Document Type :
Electronic Resource
Full Text :
https://doi.org/10.1016.j.ejps.2021.105812