Deactivation of Anti-cancer Drug Letrozole to a Carbinol Metabolite by Polymorphic Cytochrome P450 2A6 in Human Liver Microsomes

Overview

Journal Xenobiotica

Publisher Informa Healthcare

Specialties Biochemistry
Toxicology

Date 2009 Oct 23

PMID 19845430

Citations 22

Authors

K Murai

H Yamazaki

K Nakagawa

R Kawai

T Kamataki

Affiliations

Soon will be listed here.

Abstract

Cytochromes P450 (P450) involved in letrozole metabolism were investigated. Among 13 recombinant P450 forms examined, only P450 2A6 and 3A4 showed activities in transforming letrozole to its carbinol metabolite with small K(m) and high Vmax values yielding apparent Vmax/K(m) values of 0.48 and 0.24 nl min(-1) nmol(-1) P450, respectively. The metabolic activities of individual human liver microsomes showed a significant correlation with coumarin 7-hydroxylase activities (P450 2A6 marker) at a letrozole concentration of 0.5 microM, while a good correlation was also seen with testosterone 6beta-hydroxylase activities (P450 3A4 marker) at 5 microM substrate concentration with different inhibition by 8-methoxypsolaren. Significantly low carbinol-forming activities were seen in human liver microsomes from individuals possessing CYP2A6*4/*4 (whole CYP2A6 gene deletion) at a letrozole concentration of 0.5 microM. A Vmax/K(m) value measured for CYP2A6.7 (amino acid substitution type) in human liver microsomes, in the presence of anti-P450 3A4 antibodies, was approximately seven-fold smaller than that for CYP2A6.1 (wild-type). These results demonstrate that P450 2A6 and 3A4 catalyse the conversion of letrozole to its carbinol metabolite in vitro at low and high concentrations of letrozole. Polymorphic variation of CYP2A6 is considered to be relevant to inter-subject variation in therapeutic exposure of letrozole.

Citing Articles

Pharmacogenetics of Breast Cancer Treatments: A Sub-Saharan Africa Perspective.

Nthontho K, Ndlovu A, Sharma K, Kasvosve I, Hertz D, Paganotti G Pharmgenomics Pers Med. 2022; 15:613-652.

PMID: 35761855 PMC: 9233488. DOI: 10.2147/PGPM.S308531.

Analyses of nicotine metabolism biomarker genetics stratified by sex in African and European Americans.

Chenoweth M, Cox L, Nollen N, Ahluwalia J, Benowitz N, Lerman C Sci Rep. 2021; 11(1):19572.

PMID: 34599228 PMC: 8486765. DOI: 10.1038/s41598-021-98883-z.

Interactions between cardiology and oncology drugs in precision cardio-oncology.

Kamaraju S, Mohan M, Zaharova S, Wallace B, McGraw J, Lokken J Clin Sci (Lond). 2021; 135(11):1333-1351.

PMID: 34076246 PMC: 8984624. DOI: 10.1042/CS20200309.

Gender-based differences in brain and plasma pharmacokinetics of letrozole in sprague-dawley rats: Application of physiologically-based pharmacokinetic modeling to gain quantitative insights.

Arora P, Gudelsky G, Desai P PLoS One. 2021; 16(4):e0248579.

PMID: 33798227 PMC: 8018653. DOI: 10.1371/journal.pone.0248579.

How Can Drug Metabolism and Transporter Genetics Inform Psychotropic Prescribing?.

Henriques B, Yang E, Lapetina D, Carr M, Yavorskyy V, Hague J Front Genet. 2020; 11:491895.

PMID: 33363564 PMC: 7753050. DOI: 10.3389/fgene.2020.491895.