In vivo analysis of efavirenz metabolism in individuals with impaired CYP2A6 function

Julia di Iulio; Aurélie Fayet; Mona Arab-Alameddine; Margalida Rotger; Rubin Lubomirov; Matthias Cavassini; Hansjakob Furrer; Huldrych F Günthard; Sara Colombo; Chantal Csajka; Chin B Eap; Laurent A Decosterd; Amalio Telenti; Swiss HIV Cohort Study

doi:10.1097/FPC.0b013e328328d577

In vivo analysis of efavirenz metabolism in individuals with impaired CYP2A6 function

Pharmacogenet Genomics. 2009 Apr;19(4):300-9. doi: 10.1097/FPC.0b013e328328d577.

Authors

Julia di Iulio¹, Aurélie Fayet, Mona Arab-Alameddine, Margalida Rotger, Rubin Lubomirov, Matthias Cavassini, Hansjakob Furrer, Huldrych F Günthard, Sara Colombo, Chantal Csajka, Chin B Eap, Laurent A Decosterd, Amalio Telenti; Swiss HIV Cohort Study

Collaborators

Swiss HIV Cohort Study:
M Battegay, E Bernasconi, J Böni, H C Bucher, Ph Bürgisser, A Calmy, S Cattacin, M Cavassini, R Dubs, M Egger, L Elzi, M Fischer, M Flepp, A Fontana, P Francioli, H Furrer, C Fux, M Gorgievski, H Günthard, H Hirsch, B Hirschel, I Hösli, Ch Kahlert, L Kaiser, U Karrer, C Kind, Th Klimkait, B Ledergerber, G Martinetti, B Martinez, N Müller, D Nadal, M Opravil, F Paccaud, G Pantaleo, A Rauch, S Regenass, M Rickenbach, C Rudin, P Schmid, D Schultze, J Schüpbach, R Speck, P Taffé, A Telenti, A Trkola, P Vernazza, R Weber, S Yerly

Affiliation

¹ Institute of Microbiology Division of Clinical Pharmacology, University Hospital Center, University of Lausanne, Lausanne, Switzerland.

PMID: 19238117
DOI: 10.1097/FPC.0b013e328328d577

Abstract

Introduction: The antiretroviral drug efavirenz (EFV) is extensively metabolized into three primary metabolites: 8-hydroxy-EFV, 7-hydroxy-EFV and N-glucuronide-EFV. There is a wide interindividual variability in EFV plasma exposure, explained to a great extent by cytochrome P450 2B6 (CYP2B6), the main isoenzyme responsible for EFV metabolism and involved in the major metabolic pathway (8-hydroxylation) and to a lesser extent in 7-hydroxylation. When CYP2B6 function is impaired, the relevance of CYP2A6, the main isoenzyme responsible for 7-hydroxylation may increase. We hypothesize that genetic variability in this gene may contribute to the particularly high, unexplained variability in EFV exposure in individuals with limited CYP2B6 function.

Methods: This study characterized CYP2A6 variation (14 alleles) in individuals (N=169) previously characterized for functional variants in CYP2B6 (18 alleles). Plasma concentrations of EFV and its primary metabolites (8-hydroxy-EFV, 7-hydroxy-EFV and N-glucuronide-EFV) were measured in different genetic backgrounds in vivo.

Results: The accessory metabolic pathway CYP2A6 has a critical role in limiting drug accumulation in individuals characterized as CYP2B6 slow metabolizers.

Conclusion: Dual CYP2B6 and CYP2A6 slow metabolism occurs at significant frequency in various human populations, leading to extremely high EFV exposure.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Alkynes
Alleles
Anti-HIV Agents / blood
Anti-HIV Agents / chemistry
Anti-HIV Agents / metabolism*
Anti-HIV Agents / pharmacokinetics
Aryl Hydrocarbon Hydroxylases / metabolism*
Asian People / genetics
Benzoxazines / blood
Benzoxazines / chemistry
Benzoxazines / metabolism*
Benzoxazines / pharmacokinetics
Black People / genetics
Cyclopropanes
Cytochrome P-450 CYP2A6
Gene Frequency
Genetic Variation
Hispanic or Latino / genetics
Humans
Metabolic Networks and Pathways / genetics*
Molecular Structure
Pharmacogenetics*
Polymorphism, Single Nucleotide
White People / genetics

Substances

Alkynes
Anti-HIV Agents
Benzoxazines
Cyclopropanes
Aryl Hydrocarbon Hydroxylases
CYP2A6 protein, human
Cytochrome P-450 CYP2A6
efavirenz