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大鼠、猴子和人类精子发生过程中激素调节特定位点的鉴定。

Identification of specific sites of hormonal regulation in spermatogenesis in rats, monkeys, and man.

作者信息

McLachlan R I, O'Donnell L, Meachem S J, Stanton P G, de Kretser D M, Pratis K, Robertson D M

机构信息

Prince Henry's Institute of Medical Research, Monash Medical Centre, Clayton, Victoria, Australia.

出版信息

Recent Prog Horm Res. 2002;57:149-79. doi: 10.1210/rp.57.1.149.

Abstract

A detailed understanding of the hormonal regulation of spermatogenesis is required for the informed assessment and management of male fertility and, conversely, for the development of safe and reversible male hormonal contraception. An approach to the study of these issues is outlined based on the use of well-defined in vivo models of gonadotropin/androgen deprivation and replacement, the quantitative assessment of germ cell number using stereological techniques, and the directed study of specific steps in spermatogenesis shown to be hormone dependent. Drawing together data from rat, monkey, and human models, we identify differences between species and formulate an overview of the hormonal regulation of spermatogenesis. There is good evidence for both separate and synergistic roles for both testosterone and follicle-stimulating hormone (FSH) in achieving quantitatively normal spermatogenesis. Based on relatively selective withdrawal and replacement studies, FSH has key roles in the progression of type A to B spermatogonia and, in synergy with testosterone, in regulating germ cell viability. Testosterone is an absolute requirement for spermatogenesis. In rats, it has been shown to promote the adhesion of round spermatids to Sertoli cells, without which they are sloughed from the epithelium and spermatid elongation fails. The release of mature elongated spermatids from the testis (spermiation) is also under FSH/testosterone control in rats. Data from monkeys and men treated with steroidal contraceptives indicate that impairment of spermiation is a key to achieving azoospermia. The contribution of 5alpha-reduced androgens in the testis to the regulation of spermatogenesis is also relevant, as 5alpha-reduced androgens are maintained during gonadotropin suppression and may act to maintain low levels of germ cell development. These concepts are also discussed in the context of male hormonal contraceptive development.

摘要

要对男性生育能力进行明智的评估和管理,以及反过来开发安全且可逆的男性激素避孕方法,都需要对精子发生的激素调节有详细的了解。基于使用明确的促性腺激素/雄激素剥夺和替代的体内模型、使用体视学技术对生殖细胞数量进行定量评估,以及对精子发生中显示为激素依赖性的特定步骤进行定向研究,概述了研究这些问题的方法。综合大鼠、猴子和人类模型的数据,我们确定了物种之间的差异,并对精子发生的激素调节进行了概述。有充分证据表明,睾酮和促卵泡激素(FSH)在实现定量正常的精子发生中既起单独作用又起协同作用。基于相对选择性的撤药和替代研究,FSH在A型到B型精原细胞的进展中起关键作用,并且与睾酮协同作用,调节生殖细胞的活力。睾酮是精子发生的绝对必要条件。在大鼠中,已证明它能促进圆形精子细胞与支持细胞的黏附,没有这种黏附,它们就会从上皮脱落,精子细胞伸长失败。在大鼠中,成熟伸长精子细胞从睾丸的释放(精子排出)也受FSH/睾酮控制。来自接受甾体避孕药治疗的猴子和男性的数据表明,精子排出受损是实现无精子症的关键。睾丸中5α-还原雄激素对精子发生调节的贡献也很重要,因为在促性腺激素抑制期间5α-还原雄激素会维持,并且可能起到维持低水平生殖细胞发育的作用。这些概念也在男性激素避孕开发的背景下进行了讨论。

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