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促卵泡激素对体外培养的胎鼠睾丸基础睾酮分泌及促黄体生成素刺激的睾酮分泌的刺激作用。

Stimulatory effect of follicle-stimulating hormone on basal and luteinizing hormone-stimulated testosterone secretions by the fetal rat testis in vitro.

作者信息

Lecerf L, Rouiller-Fabre V, Levacher C, Gautier C, Saez J M, Habert R

机构信息

INSERM U-307, Université Paris 7, France.

出版信息

Endocrinology. 1993 Nov;133(5):2313-8. doi: 10.1210/endo.133.5.8404683.

Abstract

The in vitro effect of FSH on testosterone secretion by the fetal rat testis was studied. Testes were cultured in the presence or absence of either commercial human (h) FSH (Metrodine; 200 mIU/ml) or recombinant hFSH (200 mIU/ml) for 3 days and with 100 ng/ml ovine LH during the last 4 h of culture. To avoid a stimulatory effect by the 0.4% LH that contaminates Metrodine, the cultures were performed in the presence of a monoclonal anti-hLH beta antibody and with a concentration of Metrodine that had no short term stimulatory effect on testosterone production by the fetal testes in vitro. Metrodine treatment had a positive long term effect on both basal and LH-stimulated testosterone secretion by fetal testes explanted on days 18.5, 20.5, and 22.5 postconception, which was abolished by the addition of a monoclonal anti-hFSH beta antibody. LH-free recombinant FSH also augmented basal and LH-stimulated testosterone secretion of testes explanted on days 13.5, 14.5, and 18.5 postconception. The positive effect of recombinant hFSH appeared during the second day of treatment with day 14.5 and 18.5 testes and on the third day of treatment with day 13.5 testes. As it is widely accepted that FSH receptors are exclusively localized on Sertoli cells, these results suggest that on or before day 15.5 of fetal life, 1) Sertoli cells are able to respond to FSH, 2) Sertoli cells can produce factors that are able to act on Leydig cell function, and 3) Leydig cells are sensitive to FSH-induced Sertoli cell factors. In conclusion, this study points out a potential paracrine control of fetal Leydig cell function and/or differentiation by fetal Sertoli cells as soon as fetal Leydig cells differentiate.

摘要

研究了促卵泡激素(FSH)对胎鼠睾丸睾酮分泌的体外作用。将睾丸在存在或不存在市售人(h)FSH(美曲普明;200 mIU/ml)或重组hFSH(200 mIU/ml)的情况下培养3天,并在培养的最后4小时加入100 ng/ml绵羊促黄体生成素(LH)。为避免美曲普明中0.4%的LH产生刺激作用,培养在单克隆抗hLHβ抗体存在下进行,且美曲普明的浓度对体外胎鼠睾丸睾酮产生无短期刺激作用。美曲普明处理对受孕后第18.5、20.5和22.5天取出的胎鼠睾丸的基础和LH刺激的睾酮分泌有长期积极作用,加入单克隆抗hFSHβ抗体可消除这种作用。无LH的重组FSH也增加了受孕后第13.5、14.5和18.5天取出的睾丸的基础和LH刺激的睾酮分泌。重组hFSH的积极作用在第14.5和18.5天睾丸处理的第二天以及第13.5天睾丸处理的第三天出现。由于普遍认为FSH受体仅定位于支持细胞,这些结果表明在胎儿生命的第15.5天及之前,1)支持细胞能够对FSH作出反应,2)支持细胞能够产生作用于睾丸间质细胞功能的因子,3)睾丸间质细胞对FSH诱导的支持细胞因子敏感。总之,本研究指出,一旦胎儿睾丸间质细胞分化,胎儿支持细胞可能对胎儿睾丸间质细胞功能和/或分化进行旁分泌控制。

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