Regulation of Testosterone Hydroxylation by Rat Liver Microsomal Cytochrome P-450

Overview

Journal Arch Biochem Biophys

Publisher Elsevier

Specialties Biochemistry
Biophysics

Date 1987 May 15

PMID 3592665

Citations 29

Authors

A J Sonderfan

M P Arlotto

D R Dutton

S K McMillen

A Parkinson

Affiliations

Soon will be listed here.

Abstract

The pathways of testosterone oxidation catalyzed by purified and membrane-bound forms of rat liver microsomal cytochrome P-450 were examined with an HPLC system capable of resolving 14 potential hydroxylated metabolites of testosterone and androstenedione. Seven pathways of testosterone oxidation, namely the 2 alpha-, 2 beta-, 6 beta-, 15 beta-, 16 alpha-, and 18-hydroxylation of testosterone and 17-oxidation to androstenedione, were sexually differentiated in mature rats (male/female = 7-200 fold) but not in immature rats. Developmental changes in two cytochrome P-450 isozymes largely accounted for this sexual differentiation. The selective expression of cytochrome P-450h in mature male rats largely accounted for the male-specific, postpubertal increase in the rate of testosterone 2 alpha-, 16 alpha, and 17-oxidation, whereas the selective repression of cytochrome P-450p in female rats accounted for the female-specific, postpubertal decline in testosterone 2 beta-, 6 beta-, 15 beta-, and 18-hydroxylase activity. A variety of cytochrome P-450p inducers, when administered to mature female rats, markedly increased (up to 130-fold) the rate of testosterone 2 beta-, 6 beta-, 15 beta-, and 18-hydroxylation. These four pathways of testosterone hydroxylation were catalyzed by partially purified cytochrome P-450p, and were selectively stimulated when liver microsomes from troleandomycin- or erythromycin estolate-induced rats were treated with potassium ferricyanide, which dissociates the complex between cytochrome P-450p and these macrolide antibiotics. Just as the testosterone 2 beta-, 6 beta-, 15 beta-, and 18-hydroxylase activity reflected the levels of cytochrome P-450p in rat liver microsomes, so testosterone 7 alpha-hydroxylase activity reflected the levels of cytochrome P-450a; 16 beta-hydroxylase activity the levels of cytochrome P-450b; and 2 alpha-hydroxylase activity the levels of cytochrome P-450h. It is concluded that the regio- and stereoselective hydroxylation of testosterone provides a functional basis to study simultaneously the regulation of several distinct isozymes of rat liver microsomal cytochrome P-450.

Citing Articles

A 2024 inventory of test methods relevant to thyroid hormone system disruption for human health and environmental regulatory hazard assessment.

Vergauwen L, Bajard L, Tait S, Langezaal I, Sosnowska A, Roncaglioni A Open Res Eur. 2025; 4:242.

PMID: 39931575 PMC: 11809485. DOI: 10.12688/openreseurope.18739.1.

Physiological Responses of Earthworm Under Acid Rain Stress.

Chen X, Zhang J, Wei H Int J Environ Res Public Health. 2020; 17(19).

PMID: 33023052 PMC: 7579360. DOI: 10.3390/ijerph17197246.

modulatory effects of , arjunic acid, arjunetin and arjungenin on CYP3A4, CYP2D6 and CYP2C9 enzyme activity in human liver microsomes.

Varghese A, Savai J, Pandita N, Gaud R Toxicol Rep. 2017; 2:806-816.

PMID: 28962416 PMC: 5598323. DOI: 10.1016/j.toxrep.2015.02.008.

In Vitro Evaluation of Reversible and Time-Dependent Inhibitory Effects of Kalanchoe crenata on CYP2C19 and CYP3A4 Activities.

Awortwe C, Manda V, Avonto C, Khan S, Khan I, Walker L Drug Metab Lett. 2015; 9(1):48-62.

PMID: 25600201 PMC: 5656046. DOI: 10.2174/1872312809666150119110200.

Confounding factors and genetic polymorphism in the evaluation of individual steroid profiling.

Kuuranne T, Saugy M, Baume N Br J Sports Med. 2014; 48(10):848-55.

PMID: 24764553 PMC: 4033181. DOI: 10.1136/bjsports-2014-093510.