Minipig and Human Metabolism of Aldehyde Oxidase Substrates: In Vitro–In Vivo Comparisons

被引:0
|
作者
David J. Wilkinson
Rosalind L. Southall
Mingguang Li
Lisa M. Wright
Lindsay J. Corfield
Thomas A. Heeley
Benjamin Bratby
Ranbir Mannu
Sarah L. Johnson
Victoria Shaw
Holly L. Friett
Louise A. Blakeburn
John S. Kendrick
Michael B. Otteneder
机构
[1] Covance Laboratories Ltd.,Department of Metabolism
[2] Covance Laboratories Inc.,Department of Drug Metabolism
[3] Covance Laboratories Ltd.,Department of Bioanalysis
[4] Roche Innovation Center Basel,Pharmaceutical Sciences, Roche Pharmaceutical Research and Early Development
来源
The AAPS Journal | 2017年 / 19卷
关键词
aldehyde oxidase; animal models; prediction; minipig;
D O I
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中图分类号
学科分类号
摘要
The importance of aldehyde oxidase (AOX) is becoming increasingly recognized in the prediction of human pharmacokinetic parameters from animal data. The objectives of these studies were to ascertain whether an in vitro–in vivo correlation existed in the clearance and metabolic pathways of AOX substrates and to establish whether the minipig represented an appropriate non-rodent model for man in the pre-clinical development of drugs metabolized by AOX. Using the AOX substrates carbazeran, 6-deoxypenciclovir and zaleplon, clearance was estimated from in vitro depletion experiments with minipig and human liver cytosol and microsomes and scaled before comparison with data generated in parallel in vivo studies in minipigs. In vitro and in vivo metabolic pathways were characterized by LC–MS/MS. Scaling of in vitro metabolism data to predict in vivo clearance underestimated in vivo values, although the rank order of clearance for the three compounds was preserved. Prediction of human in vivo clearance from scaled minipig in vivo data produced results which correlated well with published clinical values. Overall, this study is the first to compare minipig in vitro metabolism data with in vivo pharmacokinetic data for compounds metabolized by AOX and provides a scientific rationale for the selection of this species as a model for humans in the development of drugs which are substrates of AOX.
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页码:1163 / 1174
页数:11
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