TESTOSTERONE Δ4-REDUCTASE ACTIVITY IN RAT LIVER: HORMONAL CONTROL IN VIVO

Abstract
SUMMARY: The rate-limiting step in the metabolism of testosterone by the liver is reduction of the double bond in ring A. Using a spectrophotometric assay we have studied the effects of some hormonal manipulations on the levels (per mg protein) of testosterone Δ4-reductase activity in rat liver. While the levels of enzyme activity were higher for adult female rat liver than for adult male liver, there were no further changes in livers from female rats at day 15 of gestation. In male rats, castration increased, hypophysectomy decreased and adrenalectomy had no effect on the level of activity. Administration of oestradiol valerate increased the activity in intact and adrenalectomized animals and had no effect in the hypophysectomized or castrated groups. Administration of testosterone enanthate decreased the levels of activity in the castrated and adrenalectomized groups and had no effects in unoperated or hypophysectomized animals. When given together, the two hormones were antagonistic. Prolactin had no significant effects in either intact or hypophysectomized animals. Experiments with actinomycin D and cycloheximide indicated that the synthesis of new protein was involved in the effects of oestradiol in intact rats. All the changes reflected alterations in the microsomal enzyme level.

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