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促性腺激素、激活素A和胰岛素样生长因子-1受体对培养的人颗粒黄体细胞中免疫反应性抑制素A和B分泌的调节

Regulation of immunoreactive inhibin A and B secretion in cultured human granulosa-luteal cells by gonadotropins, activin A and insulin-like growth factor type-1 receptor.

作者信息

Vänttinen T, Liu J, Liu J, Hydén-Granskog C, Parviainen M, Penttilä I, Voutilainen R

机构信息

Department of Pediatrics, Kuopio University Hospital, Kuopio, Finland.

出版信息

J Endocrinol. 2000 Nov;167(2):289-94. doi: 10.1677/joe.0.1670289.

Abstract

Inhibins are gonadal glycoproteins with endocrine effects on pituitary FSH secretion and para/autocrine effects on ovarian and testicular function. The purpose of this study was to investigate the endocrine and para/autocrine regulation of inhibin A and inhibin B secretion in human ovarian granulosa-luteal cells. The cells were obtained from women undergoing in vitro fertilization, and the primary cultures were treated with FSH, LH, human chorionic gonadotropin (hCG), activin A, 8-bromo cyclic AMP (8-BrcAMP), staurosporine (a protein kinase C inhibitor) and an antagonist of IGF action (type-1 IGF receptor antibody alpha IR3). The secretion of inhibins was measured by ELISA assays capable of reliably distinguishing between inhibin A and B. FSH, LH, hCG and 8-BrcAMP increased inhibin A secretion on average up to 180% (P<0.01), 192% (P<0.05), 210% (P<0.01) and 243% (P<0.01) respectively of the control level, while their stimulatory effect on inhibin B secretion was less pronounced (up to 167%, P<0.01; 139%, P<0.05; 127%, P>0.05; 133%, P>0.05 of the controls respectively). alpha IR3 decreased inhibin A and B secretion down to 70% (P<0.01) and 50% (P<0.01) respectively of the control. Staurosporine decreased inhibin B secretion down to 49% (P<0.01) of the control; its effect on inhibin A secretion was not significant. Activin A increased inhibin B secretion up to fourfold of the control (P<0.05) while its effect on inhibin A secretion was insignificant. We conclude that gonadotropins via the protein kinase A signal transduction pathway are the main positive regulators of inhibin A and B secretion in human granulosa-luteal cells. The protein kinase C signal transduction pathway seems to be important especially for inhibin B secretion. Locally produced IGFs are probably important inducers of the production of both forms of inhibin in human ovaries while activins seem to upregulate inhibin B secretion.

摘要

抑制素是一种性腺糖蛋白,对垂体促卵泡激素(FSH)分泌具有内分泌作用,对卵巢和睾丸功能具有旁分泌/自分泌作用。本研究旨在探讨人卵巢颗粒黄体细胞中抑制素A和抑制素B分泌的内分泌及旁分泌/自分泌调节机制。细胞取自接受体外受精的女性,原代培养物分别用促卵泡激素(FSH)、促黄体生成素(LH)、人绒毛膜促性腺激素(hCG)、激活素A、8-溴环磷酸腺苷(8-BrcAMP)、星形孢菌素(一种蛋白激酶C抑制剂)以及胰岛素样生长因子(IGF)作用拮抗剂(1型IGF受体抗体αIR3)进行处理。采用能够可靠区分抑制素A和B的酶联免疫吸附测定(ELISA)法检测抑制素的分泌。FSH、LH、hCG和8-BrcAMP使抑制素A分泌平均分别增加至对照水平的180%(P<0.01)、192%(P<0.05)、210%(P<0.01)和243%(P<0.01),而它们对抑制素B分泌的刺激作用则不那么明显(分别为对照的167%,P<0.01;139%,P<0.05;127%,P>0.05;133%,P>0.05)。αIR3使抑制素A和B分泌分别降至对照的70%(P<0.01)和50%(P<0.01)。星形孢菌素使抑制素B分泌降至对照的49%(P<0.01);其对抑制素A分泌的影响不显著。激活素A使抑制素B分泌增加至对照的四倍(P<0.05),而其对抑制素A分泌的影响不显著。我们得出结论,促性腺激素通过蛋白激酶A信号转导途径是人类颗粒黄体细胞中抑制素A和B分泌的主要正调节因子。蛋白激酶C信号转导途径似乎尤其对抑制素B分泌很重要。局部产生的IGF可能是人类卵巢中两种形式抑制素产生的重要诱导剂,而激活素似乎上调抑制素B的分泌。

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