Biopharmaceutics & Drug Disposition 2011-10-01

In vitro identification of the human cytochrome p450 enzymes involved in the oxidative metabolism of loxapine.

Jiang Ping Luo, Sarvesh C Vashishtha, Edward M Hawes, Gordon McKay, Kamal K Midha, Jim Fang

Index: Biopharm. Drug Dispos. 32(7) , 398-407, (2011)

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Abstract

In vitro studies were conducted to identify the hepatic cytochrome P450 (CYP) enzymes responsible for the oxidative metabolism of loxapine to 8-hydroxyloxapine, 7-hydroxyloxapine, N-desmethylloxapine (amoxapine) and loxapine N-oxide. These studies included use of cDNA-expressed enzymes, correlation analysis with 12 phenotyped human liver microsomal samples, and use of selective inhibitors of cytochrome P450s. The resultant data indicated that loxapine was mainly metabolized by human liver microsomes to (i) 8-hydroxyloxapine by CYP1A2, (ii) 7-hydroxyloxapine by CYP2D6, (iii) N-desmethyloxapine by CYP3A4 and (iv) loxapine N-oxide by CYP3A4. The involvement of flavin-containing monooxygenase (FMO) in the formation of loxapine N-oxide was also observed.Copyright © 2011 John Wiley & Sons, Ltd.


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