Effects of cyproterone on the steroid biosynthesis in the human ovary in vitro.

Endokrinologie Pub Date : 1982-11-01
P Schürenkämper, K Lisse
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Abstract

To examine the direct effects of cyproterone on the ovarian biosynthesis of steroids, tissue slices obtained from two cyclically functional human ovaries were incubated with [4-14C]pregnenolone as precursor. The steroid production was determined by measuring the concentration of eleven 14C-labelled steroids in the medium at the end of a 3-h incubation. Under control conditions, the in vitro-synthesis of 17 alpha-hydroxypregnenolone, dehydroepiandrosterone, androstenediol (5-ene-3 beta-hydroxy-steroids) and androstenedione represents the characteristic profile of steroids of the ovary from the follicular phase. The addition of cyproterone to the incubation medium inhibited the biosynthesis of androstenedione, whereas 17 alpha-hydroxypregnenolone and dehydroepiandrosterone increased. The in vitro-synthesis of progesterone, 17 alpha-hydroxyprogesterone, oestrone and oestradiol-17 beta represents the characteristic profile of steroids of the luteal ovary. The biosynthesis of progesterone, 17 alpha-hydroxyprogesterone and oestradiol-17 beta is inhibited by cyproterone. The principal manifestation of the effects of cyproterone on the two different profiles of steroids is an apparent inhibition of the 3 beta-hydroxysteroiddehydrogenase-delta 5-4-isomerase activity. It is noteworthy, that the effects of the "pure antiandrogen" cyproterone are similar to those effects previously published for progestagens (chlormadinone acetate, norethisterone acetate and D-norgestrel). A simplified concept of the direct effects of cyproterone and progestagens on the steroidogenesis in the human ovary is proposed. The results indicate, that cyproterone, in addition to its well-known androgen receptor blocking effect, act directly on the steroid biosynthesis in the human ovary in vitro.

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环丙孕酮对体外卵巢类固醇生物合成的影响。
为了研究环丙孕酮对卵巢类固醇生物合成的直接影响,我们用[4-14C]孕烯醇酮作为前体,从两个周期功能正常的人卵巢中获得组织切片。在3小时孵育结束时,通过测量培养基中11种14c标记类固醇的浓度来确定类固醇的产生。在对照条件下,17 α -羟基孕烯醇酮、脱氢表雄酮、雄烯二醇(5-烯-3 β -羟基类固醇)和雄烯二酮的体外合成代表了卵泡期卵巢类固醇的特征。在培养液中添加环丙孕酮抑制雄烯二酮的生物合成,而17 α -羟基孕烯醇酮和脱氢表雄酮的生物合成增加。孕酮、17 α -羟孕酮、雌酮和雌二醇-17 β的体外合成代表了黄体卵巢类固醇的特征。孕酮、17 α -羟孕酮和雌二醇-17 β的生物合成被环丙孕酮抑制。环丙孕酮对两种不同类型类固醇的作用的主要表现是对3 -羟基甾体脱氢酶- 5-4异构酶活性的明显抑制。值得注意的是,“纯抗雄激素”环丙孕酮的作用与先前发表的孕激素(醋酸氯马地诺酮、醋酸去甲睾酮和d -诺孕酮)的作用相似。本文提出了环丙孕酮和孕激素对卵巢甾体形成直接影响的简化概念。结果表明,环丙孕酮除了其众所周知的雄激素受体阻断作用外,还直接作用于体外人卵巢内类固醇的生物合成。
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