The Contribution of Hepatic Inactivation of Testosterone to the Lowering of Serum Testosterone Levels by Ketoconazole

doi:10.1093/toxsci/54.1.128

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Toxicological Sciences 54, 128-137 (2000)
Copyright © 2000 by the Society of Toxicology

The Contribution of Hepatic Inactivation of Testosterone to the Lowering of Serum Testosterone Levels by Ketoconazole

Vickie S. Wilson and Gerald A. LeBlanc¹

Department of Toxicology, North Carolina State University, Raleigh, North Carolina 27695

Hepatic biotransformation processes can be modulated by chemicalexposure and these alterations can impact the biotransformationof endogenous substrates. Furthermore, chemically mediated alterationsin the biotransformation of endogenous steroid hormones havebeen implicated as a mechanism by which steroid hormone homeostasiscan be disrupted. The fungicide ketoconazole has been shownto lower serum testosterone levels and alter both gonadal synthesisand hepatic inactivation of testosterone. The present studyexamined whether the effects of ketoconazole on the hepaticbiotransformation of testosterone contribute to its loweringof serum testosterone levels. Results also were used to validatefurther the use of the androgen-regulated hepatic testosterone6 ${alpha}$ /15 ${alpha}$ -hydroxylase ratio as an indicator of androgen status. MaleCD-1 mice were fed from 0 to 160 mg/kg ketoconazole in honey.Four h after the initial treatment, serum testosterone levels,gonadal testosterone secretion, and hepatic testosterone hydroxylaseactivity decreased, and the hepatic testosterone 6 ${alpha}$ /15 ${alpha}$ -hydroxylaseratio increased in a dose-dependent manner. Immunoblot analysisindicated that the transient decline in hepatic biotransformationwas not due to reduced P450 protein levels. Rather, hepatictestosterone biotransformation activities were found to be differentiallysusceptible to direct inhibition by ketoconazole. Differentialinhibition was also responsible for the increase seen in the6 ${alpha}$ /15 ${alpha}$ -hydroxylase ratio. The changes in serum testosterone levelscould be explained by decreased gonadal synthesis of testosteroneand were not impacted by decreased hepatic biotransformationof testosterone. These results demonstrate that changes in thehepatic hydroxylation of testosterone by ketoconazole, and perhapsother chemicals, have little or no influence serum testosteronelevels.

Key Words: androgen disruption; hepatic biotransformation; ketoconazole; mice; testosterone.

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