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培养的大鼠垂体分散细胞中孕酮对促性腺激素分泌的调节。IV. 促卵泡激素的合成与释放。

Progesterone modulation of gonadotropin secretion by dispersed rat pituitary cells in culture. IV. Follicle-stimulating hormone synthesis and release.

作者信息

Krey L C, Padmanabhan V, Beitins I Z

机构信息

Laboratory of Neuroendocrinology, Rockefeller University, New York, NY 10021.

出版信息

Mol Cell Endocrinol. 1993 Feb;91(1-2):13-20. doi: 10.1016/0303-7207(93)90249-j.

Abstract

Estradiol-treated, rat pituitary cells were studied to examine the effects of progesterone (P) on follicle-stimulating hormone (FSH) synthesis and secretion. Progesterone was administered prior to or concurrent with 3 h secretory challenges with either gonadotropin-releasing hormone (GnRH), the iontophore A23187, the protein kinase C activator phorbol 12,13-myristate (PMA), or no secretagogue. Medium FSH levels and cell FSH stores were quantified by radioimmunoassay and bioassay. Acute (< 6 h) exposures to P increased medium levels of immunoreactive and bioactive FSH following GnRH challenge without influencing total (cell + medium) values whereas chronic (9-24 h) treatments increased both parameters. Chronic P elevated total FSH levels even when no secretagogue was present. Studies with antiprogestins, 5 alpha-dihydroprogesterone and 5 alpha-reductase inhibitors revealed that this direct action of P depended on progestin receptor occupation but not on 5 alpha-reduction. These studies indicate that P selectively increases bioactive and immunoactive FSH levels, presumably by increasing FSH synthesis, and characterize the time course and cellular mechanisms of this response. To accommodate for P modulation of total FSH levels, FSH secretion was standardized as the percentage of cellular stores available for release. Progesterone modulation of GnRH-stimulated FSH secretion was multiphasic, i.e. increased at 0-6 h, unchanged at 9 h and suppressed at 24 h. Acute and chronic exposures to P similarly modulated A23187-stimulated FSH release, whereas both P treatments increased PMA-stimulated FSH secretion. In these experiments P modulated luteinizing hormone secretion in parallel fashion, suggesting that common cellular mechanisms underlie peptidergic and steroidal regulation of the secretion of both gonadotropins.

摘要

研究了经雌二醇处理的大鼠垂体细胞,以检测孕酮(P)对促卵泡激素(FSH)合成和分泌的影响。在使用促性腺激素释放激素(GnRH)、离子载体A23187、蛋白激酶C激活剂佛波醇12,13 - 肉豆蔻酸酯(PMA)进行3小时分泌刺激之前或同时给予孕酮,或不给予任何促分泌剂。通过放射免疫测定和生物测定对培养基中FSH水平和细胞FSH储存量进行定量。在GnRH刺激后,急性(<6小时)暴露于P可增加培养基中免疫反应性和生物活性FSH水平,而不影响总(细胞+培养基)值,而慢性(9 - 24小时)处理则增加了这两个参数。即使不存在促分泌剂,慢性P也会提高总FSH水平。使用抗孕激素、5α - 二氢孕酮和5α - 还原酶抑制剂的研究表明,P的这种直接作用取决于孕激素受体的占据,但不取决于5α - 还原。这些研究表明,P可能通过增加FSH合成选择性地提高生物活性和免疫活性FSH水平,并描述了这种反应的时间进程和细胞机制。为了适应P对总FSH水平的调节,FSH分泌被标准化为可用于释放的细胞储存量的百分比。孕酮对GnRH刺激的FSH分泌的调节是多相的,即在0 - 6小时增加,在9小时不变,在24小时受到抑制。急性和慢性暴露于P同样调节A23187刺激的FSH释放,而两种P处理均增加PMA刺激的FSH分泌。在这些实验中,P以平行方式调节促黄体生成素的分泌,表明共同的细胞机制是两种促性腺激素分泌的肽能和甾体调节的基础。

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