Toxicant-mediated induction of hepatic biotransformation enzymes is a mechanism by which endogenous steroid hormone metabolism and elimination may be altered. Endosulfan, an organochlorine insecticide that has been demonstrated to induce hepatic P450 biotransformation enzymes, was examined for its ability to alter the rate of steroid hormone metabolism in CD-1 mice. Our objective was to evaluate whether endosulfan-induced changes in the rate of testosterone metabolism were reflected in the rate of testosterone clearance and if those alterations were sufficient to disrupt steroid hormone homeostasis within the animal. Major pathways for testosterone metabolism in the liver, including hydroxylation, conjugation to glucuronic acid or sulfate, and reduction/dehydrogenation, were examined for changes due to endosulfan exposure. In female mice, endosulfan treatment elicited a dose-dependent increase in the rate of total testosterone hydroxyl metabolite formation by selectively increasing the rate of production of 16 beta-, 6 alpha, and 16 alpha-hydroxytestosterone metabolites. The hydroxylation of testosterone in the 16 beta position was most sensitive to endosulfan with a 3.3-fold increase in the rate of production of this metabolite observed following exposure to 7.5 mg/kg/day for 7 days. The rate of testosterone dehydrogenation to androstenedione was increased by 7.5 mg/kg/day of endosulfan, but the rate of direct glucuronic acid or sulfate conjugation to testosterone was not affected by any of the dosages investigated. Endosulfan was generally more toxic to male mice and did not significantly alter the rate of total hydroxytestosterone metabolite formation or glucuronic acid or sulfate conjugation. The ability of endosulfan to enhance the elimination of testosterone was, therefore, investigated in female mice. Exposure of mice to 7.5 mg/kg/day of endosulfan resulted in an approximately 3.6-fold increase in the rate of urinary elimination of [14C]androgen, but had no significant effect on the fecal elimination of [14C]androgen. The increase in androgen clearance was associated only with a small, nonsignificant decrease in serum testosterone levels. Results indicate that increases in testosterone biotransformation from endosulfan exposure can result in increases in the elimination of the steroid. However, homeostatic processes apparently compensate for the effect and minimize any consequences on serum hormone levels.