The importance of villous physiology and morphology in mechanistic physiologically-based pharmacokinetic models

Emile P Chen; Guoying Tai; Harma Ellens

doi:10.1007/s11095-013-1161-x

The importance of villous physiology and morphology in mechanistic physiologically-based pharmacokinetic models

Pharm Res. 2014 Feb;31(2):305-21. doi: 10.1007/s11095-013-1161-x. Epub 2013 Aug 30.

Authors

Emile P Chen¹, Guoying Tai, Harma Ellens

Affiliation

¹ Department of Preclinical Drug Metabolism and Pharmacokinetics, GlaxoSmithKline, King of Prussia, Pennsylvania, 19406, USA, emile.p.chen@gsk.com.

PMID: 23990312
DOI: 10.1007/s11095-013-1161-x

Abstract

Purpose: Existing PBPK models incorporating intestinal first-pass metabolism account for effect of drug permeability on accessible absorption surface area by use of "effective" permeability, P eff , without adjusting number of enterocytes involved in absorption or proportion of intestinal CYP3A involved in metabolism. The current model expands on existing models by accounting for these factors.

Methods: The PBPK model was developed using SAAM II. Midazolam clinical data was generated at GlaxoSmithKline.

Results: The model simultaneously captures human midazolam blood concentration profile and previously reported intestinal availability, using values for CYP3A CLu int , permeability and accessible surface area comparable to literature data. Simulations show: (1) failure to distinguish absorbing from non-absorbing enterocytes results in overestimation of intestinal metabolism of highly permeable drugs absorbed across the top portion of the villous surface only; (2) first-pass extraction of poorly permeable drugs occurs primarily in enterocytes, drugs with higher permeability are extracted by enterocytes and hepatocytes; (3) CYP3A distribution along crypt-villous axes does not significantly impact intestinal metabolism; (4) differences in permeability of perpetrator and victim drugs results in their spatial separation along the villous axis and intestinal length, diminishing drug-drug interaction magnitude.

Conclusions: The model provides a useful tool to interrogate intestinal absorption/metabolism of candidate drugs.

MeSH terms

Adult
Aged
Computer Simulation
Cytochrome P-450 CYP3A / metabolism
Drug Interactions
Enterocytes / metabolism
Female
Hepatocytes / metabolism
Humans
Intestinal Absorption
Intestinal Mucosa / metabolism
Midazolam / blood
Midazolam / pharmacokinetics*
Middle Aged
Models, Biological
Permeability

Substances

CYP3A protein, human
Cytochrome P-450 CYP3A
Midazolam