男性化编程窗口。

Endocrine development Pub Date : 2014-01-01 Epub Date: 2014-09-09 DOI:10.1159/000363609
Michelle Welsh, Hiroko Suzuki, Gen Yamada
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引用次数: 60

摘要

性别分化是一系列严格调控的事件,将性腺和生殖器转变为性别特异性结构。这是由胎儿睾丸产生的激素驱动的,主要是睾酮(T)。然而,每种结构的男性化并不是同步发生的,直到最近,人们才认为雄激素也在胎儿生命的很长一段时间内控制着这种男性化,与胎儿T产生的时期一致。然而,在雄性和雌性啮齿动物模型中发现了一个常见的胎儿雄性化编程窗口(MPW),其中雄激素必须作用于生殖道的所有组成部分,并允许它们以后的完全发育。雄激素作用受损仅在MPW内可引起隐睾和尿道下裂。这种MPW可能发生在人类妊娠8-14周之间。对转基因小鼠的研究已经开始调查其中的一些潜在机制。肛门生殖器距离可以预测无精子症、尿道下裂和隐睾等疾病的发病率,并且可以在MPW中提供雄激素作用的非侵入性终身指标,对性发育障碍患者的临床评估有用。此外,外生殖器的一些诊断特征也有助于研究这种MPW。
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The masculinization programming window.

Sexual differentiation is a tightly regulated series of events which transform the indifferent gonads and genitalia into sex-specific structures. This is driven by hormones produced by the fetal testes, primarily testosterone (T). However, masculinization of each structure does not occur synchronously and, until recently, it was presumed that androgens also control this masculinization over a broad period of fetal life, coincident with the period of fetal T production. However, a common fetal masculinization programming window (MPW) has been identified in male and female rodent models in which androgens must act to masculinize all components of the reproductive tract and allow their later complete development. Impaired androgen action only within this MPW can induce cryptorchidism and hypospadias. This MPW is likely to occur between 8-14 weeks' gestation in humans. Studies in transgenic mice have begun to investigate some of the underlying mechanisms involved. Anogenital distance is predictive of the incidence of disorders, such as azoospermia, hypospadias and cryptorchidism, and could provide a noninvasive, lifelong indicator of androgen action within this MPW, useful in clinical assessment of patients with disorders of sexual development. In addition, several diagnostic characteristics of the external genitalia are also useful in investigating this MPW.

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