Physiologically based pharmacokinetic model of mechanism-based inhibition of CYP3A by clarithromycin

Physiologically based pharmacokinetic model of mechanism-based inhibition of CYP3A by clarithromycin

The prediction of clinical drug-drug interactions (DDIs) due to mechanism-based inhibitors of CYP3A is complicated when the inhibitor itself is metabolized by CYP3A, as in the case of clarithromycin. Previous attempts to predict the effects of clarithromycin on CYP3A substrates, e.g., midazolam, fai...

Full description

Saved in:
Bibliographic Details
Main Authors: Quinney S.K., Zhang X., Lucksiri A., Gorski J.C., Li L., Hall S.D.
Format: Article
Language:English
Published: 2014
Online Access:http://www.scopus.com/inward/record.url?eid=2-s2.0-76149083862&partnerID=40&md5=474c87e21322e9d8b54c62945acb791f
http://cmuir.cmu.ac.th/handle/6653943832/4621
Tags: Add Tag
No Tags, Be the first to tag this record!
Institution: Chiang Mai University
Language: English
id th-cmuir.6653943832-4621
record_format dspace
spelling th-cmuir.6653943832-46212014-08-30T02:42:40Z Physiologically based pharmacokinetic model of mechanism-based inhibition of CYP3A by clarithromycin Quinney S.K. Zhang X. Lucksiri A. Gorski J.C. Li L. Hall S.D. The prediction of clinical drug-drug interactions (DDIs) due to mechanism-based inhibitors of CYP3A is complicated when the inhibitor itself is metabolized by CYP3A, as in the case of clarithromycin. Previous attempts to predict the effects of clarithromycin on CYP3A substrates, e.g., midazolam, failed to account for nonlinear metabolism of clarithromycin. A semiphysiologically based pharmacokinetic model was developed for clarithromycin and midazolam metabolism, incorporating hepatic and intestinal metabolism by CYP3A and non-CYP3A mechanisms. CYP3A inactivation by clarithromycin occurred at both sites.KI and kinact values for clarithromycin obtained from in vitro sources were unable to accurately predict the clinical effect of clarithromycin on CYP3A activity. An iterative approach determined the optimum values to predict in vivo effects of clarithromycin on midazolam to be 5.3μMfor Ki and 0.4 and 4 h-1 for kinact in the liver and intestines, respectively. The incorporation of CYP3A-dependent metabolism of clarithromycin enabled prediction of its nonlinear pharmacokinetics. The predicted 2.6-fold change in intravenous midazolam area under the plasma concentration-time curve (AUC) after 500 mg of clarithromycin orally twice daily was consistent with clinical observations. Although the mean predicted 5.3-fold change in the AUC of oral midazolam was lower than mean observed values, it was within the range of observations. Intestinal CYP3A activity was less sensitive to changes inKI, kinact, and CYP3A half-life than hepatic CYP3A. This semiphysiologically based pharmacokinetic model incorporating CYP3A inactivation in the intestine and liver accurately predicts the nonlinear pharmacokinetics of clarithromycin and the DDI observed between clarithromycin and midazolam. Furthermore, this model framework can be applied to other mechanism-based inhibitors. Copyright © 2010 by The American Society for Pharmacology and Experimental Therapeutics. 2014-08-30T02:42:40Z 2014-08-30T02:42:40Z 2010 Article 909556 10.1124/dmd.109.028746 19884323 DMDSA http://www.scopus.com/inward/record.url?eid=2-s2.0-76149083862&partnerID=40&md5=474c87e21322e9d8b54c62945acb791f http://cmuir.cmu.ac.th/handle/6653943832/4621 English
institution Chiang Mai University
building Chiang Mai University Library
country Thailand
collection CMU Intellectual Repository
language English
description The prediction of clinical drug-drug interactions (DDIs) due to mechanism-based inhibitors of CYP3A is complicated when the inhibitor itself is metabolized by CYP3A, as in the case of clarithromycin. Previous attempts to predict the effects of clarithromycin on CYP3A substrates, e.g., midazolam, failed to account for nonlinear metabolism of clarithromycin. A semiphysiologically based pharmacokinetic model was developed for clarithromycin and midazolam metabolism, incorporating hepatic and intestinal metabolism by CYP3A and non-CYP3A mechanisms. CYP3A inactivation by clarithromycin occurred at both sites.KI and kinact values for clarithromycin obtained from in vitro sources were unable to accurately predict the clinical effect of clarithromycin on CYP3A activity. An iterative approach determined the optimum values to predict in vivo effects of clarithromycin on midazolam to be 5.3μMfor Ki and 0.4 and 4 h-1 for kinact in the liver and intestines, respectively. The incorporation of CYP3A-dependent metabolism of clarithromycin enabled prediction of its nonlinear pharmacokinetics. The predicted 2.6-fold change in intravenous midazolam area under the plasma concentration-time curve (AUC) after 500 mg of clarithromycin orally twice daily was consistent with clinical observations. Although the mean predicted 5.3-fold change in the AUC of oral midazolam was lower than mean observed values, it was within the range of observations. Intestinal CYP3A activity was less sensitive to changes inKI, kinact, and CYP3A half-life than hepatic CYP3A. This semiphysiologically based pharmacokinetic model incorporating CYP3A inactivation in the intestine and liver accurately predicts the nonlinear pharmacokinetics of clarithromycin and the DDI observed between clarithromycin and midazolam. Furthermore, this model framework can be applied to other mechanism-based inhibitors. Copyright © 2010 by The American Society for Pharmacology and Experimental Therapeutics.
format Article
author Quinney S.K.
Zhang X.
Lucksiri A.
Gorski J.C.
Li L.
Hall S.D.
spellingShingle Quinney S.K.
Zhang X.
Lucksiri A.
Gorski J.C.
Li L.
Hall S.D.
Physiologically based pharmacokinetic model of mechanism-based inhibition of CYP3A by clarithromycin
author_facet Quinney S.K.
Zhang X.
Lucksiri A.
Gorski J.C.
Li L.
Hall S.D.
author_sort Quinney S.K.
title Physiologically based pharmacokinetic model of mechanism-based inhibition of CYP3A by clarithromycin
title_short Physiologically based pharmacokinetic model of mechanism-based inhibition of CYP3A by clarithromycin
title_full Physiologically based pharmacokinetic model of mechanism-based inhibition of CYP3A by clarithromycin
title_fullStr Physiologically based pharmacokinetic model of mechanism-based inhibition of CYP3A by clarithromycin
title_full_unstemmed Physiologically based pharmacokinetic model of mechanism-based inhibition of CYP3A by clarithromycin
title_sort physiologically based pharmacokinetic model of mechanism-based inhibition of cyp3a by clarithromycin
publishDate 2014
url http://www.scopus.com/inward/record.url?eid=2-s2.0-76149083862&partnerID=40&md5=474c87e21322e9d8b54c62945acb791f
http://cmuir.cmu.ac.th/handle/6653943832/4621
_version_ 1681420271628582912

Similar Items