Characterization of CYP3A5 Selective Inhibitors for Reaction Phenotyping of Drug Candidates

Overview

Journal AAPS J

Specialty Pharmacology

Date 2024 Feb 17

PMID 38366061

Authors

Jie Chen

Lloyd Wei Tat Tang

Samantha Jordan

Makayla Harrison

Gabrielle M Gualtieri

Ethan DaSilva

Danial Morris

Gary Bora

Ye Che

Li Di

Affiliations

Soon will be listed here.

Abstract

CYP3A is one of the most important classes of enzymes and is involved in the metabolism of over 70% drugs. While several selective CYP3A4 inhibitors have been identified, the search for a selective CYP3A5 inhibitor has turned out to be rather challenging. Recently, several selective CYP3A5 inhibitors have been identified through high-throughput screening of ~ 11,000 compounds and hit expansion using human recombinant enzymes. We set forth to characterize the three most selective CYP3A5 inhibitors in a more physiologically relevant system of human liver microsomes to understand if these inhibitors can be used for reaction phenotyping studies in drug discovery settings. Gomisin A and T-5 were used as selective substrate reactions for CYP3A4 and CYP3A5 to determine IC values of the two enzymes. The results showed that clobetasol propionate and loteprednol etabonate were potent and selective CYP3A5 reversible inhibitors with selectivity of 24-fold against CYP3A4 and 39-fold or more against the other major CYPs. The selectivity of difluprednate in HLM is much weaker than that in the recombinant enzymes due to hydrolysis of the acetate group in HLM. Based on the selectivity data, loteprednol etabonate can be utilized as an orthogonal approach, when experimental fraction metabolized of CYP3A5 is greater than 0.5, to understand CYP3A5 contribution to drug metabolism and its clinical significance. Future endeavors to identify even more selective CYP3A5 inhibitors are warranted to enable accurate determination of CYP3A5 contribution to metabolism versus CYP3A4.

Citing Articles

CYP3A4 and CYP3A5: the crucial roles in clinical drug metabolism and the significant implications of genetic polymorphisms.

Zhang Y, Wang Z, Wang Y, Jin W, Zhang Z, Jin L PeerJ. 2024; 12:e18636.

PMID: 39650550 PMC: 11625447. DOI: 10.7717/peerj.18636.

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