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体内成年雄性大鼠附睾中雌二醇-17β对雄激素摄取、代谢及结合的抑制作用:与醋酸环丙孕酮的比较

Estradiol-17 beta inhibition of androgen uptake, metabolism and binding in epididymis of adult male rats in vivo: a comparison with cyproterone acetate.

作者信息

Tindall D J, French F S, Nayfeh S N

出版信息

Steroids. 1981 Mar;37(3):257-68. doi: 10.1016/s0039-128x(81)90244-0.

DOI:10.1016/s0039-128x(81)90244-0
PMID:6453438
Abstract

The effects of estradiol-17 beta on androgen uptake, metabolism and binding were studied in rat epididymis in vivo in comparison with cyproterone acetate. Steroids (250 ug/100 g body weight) were injected 5 min prior to 3H-testosterone in castrate rats. Estradiol-17 beta inhibited 3H-testosterone uptake into epididymal cytosol by 58% as compared to 38% by cyproterone acetate. 3H-Testosterone uptake into epididymal nuclei was inhibited 95% by estradiol-17 beta and 83% by cyproterone acetate. Total bound radioactivity in cytosol fractions was reduced to a greater extent by estradiol-17 beta than cyproterone acetate when either 3H-testosterone or 3H-dihydrotestosterone was injected. Binding of 3H-dihydrotestosterone to nuclear receptors was completely abolished by estradiol-17 beta; whereas approximately 20% binding remained in the nuclear extract after cyproterone acetate treatment. Metabolism of 3H-testosterone in vivo was also altered by estradiol-17 beta, resulting in diminished conversion to 3H-dihydrotestosterone. Cyproterone acetate, on the other hand, did not affect 3H-testosterone metabolism. Estradiol-17 beta and cyproterone acetate inhibited in vitro binding of 3H-dihydrotestosterone to the intracellular cytoplasmic receptor, but not the intraluminal androgen binding protein (ABP). These data suggest that estradiol-17 beta may have a more potent antiandrogenic effect on the epididymis than cyproterone acetate due to inhibition of 5 alpha reduction of testosterone as well as binding to the androgen receptor.

摘要

与醋酸环丙孕酮相比,在体内对大鼠附睾中雌二醇 - 17β对雄激素摄取、代谢和结合的影响进行了研究。在去势大鼠中,在注射3H - 睾酮前5分钟注射类固醇(250μg/100g体重)。与醋酸环丙孕酮抑制38%相比,雌二醇 - 17β抑制附睾细胞质中3H - 睾酮摄取达58%。雌二醇 - 17β抑制附睾细胞核中3H - 睾酮摄取95%,醋酸环丙孕酮抑制83%。当注射3H - 睾酮或3H - 双氢睾酮时,雌二醇 - 17β比醋酸环丙孕酮更能使细胞质部分的总结合放射性降低。雌二醇 - 17β完全消除了3H - 双氢睾酮与核受体的结合;而醋酸环丙孕酮处理后,核提取物中仍保留约20%的结合。雌二醇 - 17β也改变了体内3H - 睾酮的代谢,导致其向3H - 双氢睾酮的转化减少。另一方面,醋酸环丙孕酮不影响3H - 睾酮的代谢。雌二醇 - 17β和醋酸环丙孕酮在体外抑制3H - 双氢睾酮与细胞内细胞质受体的结合,但不抑制管腔内雄激素结合蛋白(ABP)。这些数据表明,由于抑制睾酮的5α还原以及与雄激素受体结合,雌二醇 - 17β对附睾可能具有比醋酸环丙孕酮更强的抗雄激素作用。

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Estradiol-17 beta inhibition of androgen uptake, metabolism and binding in epididymis of adult male rats in vivo: a comparison with cyproterone acetate.体内成年雄性大鼠附睾中雌二醇-17β对雄激素摄取、代谢及结合的抑制作用:与醋酸环丙孕酮的比较
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Androgen receptor in rat skeletal muscle: characterization and physiological variations.大鼠骨骼肌中的雄激素受体:特性与生理变化
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Acta Endocrinol (Copenh). 1985 Aug;109(4):569-76. doi: 10.1530/acta.0.1090569.

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具有抗雄激素特性的孕激素。
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Differential distribution of dihydrotestosterone and estradiol binding sites in the epididymis of the mouse. An autoradiographic study.
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