Metabolism of testosterone and progesterone by cytochrome P450 2C19 allelic variants

Author:

Takeji Shiori1,Okada Mai1,Hayashi Shu1,Kanamaru Kengo1,Uno Yuichi2,Imaishi Hiromasa3,Uno Tomohide1ORCID

Affiliation:

1. Graduate School of Agricultural Science Kobe University Kobe Japan

2. Department of Plant Resource Science Faculty of Agriculture Kobe University Kobe Japan

3. Functional Analysis of Environmental Genes Research Center for Environmental, Genomics Kobe University Kobe Japan

Abstract

AbstractCYP2C19 is a member of the human microsomal cytochrome P450 (CYP). Significant variation in CYP2C19 levels and activity can be attributed to polymorphisms in this gene. Wildtype CYP2C19 and 13 mutants (CYP2C19.1B, CYP2C19.5A, CYP2C19.5B, CYP2C19.6, CYP2C19.8, CYP2C19.9, CYP2C19.10, CYP2C19.11, CYP2C19.13, CYP2C19.16, CYP2C19.19, CYP2C19.23, CYP2C19.30, and CYP2C19.33) were coexpressed with NADPH‐cytochrome P450 reductase in Escherichia coli. Hydroxylase activity toward testosterone and progesterone was also examined. Ten CYP2C19 variants showed Soret peaks (450 nm) typical of P450 in the reduced CO‐difference spectra. CYP2C19.11 and CYP2C19.23 showed higher testosterone 11α, 16α‐/17‐ and progesterone 6β‐,21‐,16α‐/17α‐hydroxylase activities than CYP2C19.1B. CYP2C19.6, CYP2C19.16, CYP2C19.19, and CYP2C19.30 showed lower activity than CYP2C19.1B. CYP2C19.9, CYP2C19.10. CYP2C19.13, and CYP2C19.33 showed different hydroxylation activities than CYP2C19.1B. These results indicated that CYP2C19 variants have very different substrate specificities for testosterone and progesterone.

Publisher

Wiley

Subject

Pharmacology (medical),Pharmaceutical Science,Pharmacology,General Medicine

Reference49 articles.

1. Analysis of Cytochrome P450 Metabolites of Arachidonic and Linoleic Acids by Liquid Chromatography–Mass Spectrometry with Ion Trap MS2

2. Role of cytochrome P450 in estradiol metabolism in vitro;Cheng Z. N.;Acta Pharmacologica Sinica,2001

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