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激素介导的发育中大脑甾体受体的表观遗传变化:对性别分化的影响。

Hormonally mediated epigenetic changes to steroid receptors in the developing brain: implications for sexual differentiation.

机构信息

Program in Neuroscience, University of Maryland School of Medicine, Baltimore, MD, USA.

出版信息

Horm Behav. 2011 Mar;59(3):338-44. doi: 10.1016/j.yhbeh.2010.08.009. Epub 2010 Aug 25.

Abstract

The establishment of sex-specific neural morphology, which underlies sex-specific behaviors, occurs during a perinatal sensitive window in which brief exposure to gonadal steroid hormones produces permanent masculinization of the brain. In the rodent, estradiol derived from testicular androgens is a principal organizational hormone. The mechanism by which transient estradiol exposure induces permanent differences in neuronal anatomy has been widely investigated, but remains elusive. Epigenetic changes, such as DNA methylation, allow environmental influences to alter long-term gene expression patterns and therefore may be a potential mediator of estradiol-induced organization of the neonatal brain. Here we review data that demonstrate sex and estradiol-induced differences in DNA methylation on the estrogen receptor α (ERα), estrogen receptor β (ERβ), and progesterone receptor (PR) promoters in sexually dimorphic brain regions across development. Contrary to the overarching view of DNA methylation as a permanent modification directly tied to gene expression, these data demonstrate that methylation patterns on steroid hormone receptors change across the life span and do not necessarily predict expression. Although further exploration into the mechanism and significance of estradiol-induced alterations in DNA methylation patterns in the neonatal brain is necessary, these results provide preliminary evidence that epigenetic alterations can occur in response to early hormone exposure and may mediate estradiol-induced organization of sex differences in the neonatal brain.

摘要

性别特异性行为的基础是特定于性别的神经形态的建立,它发生在围产期的敏感窗口期间,在此期间,短暂暴露于性腺类固醇激素会导致大脑永久性雄性化。在啮齿动物中,来自睾丸雄激素的雌二醇是主要的组织激素。广泛研究了短暂暴露于雌二醇如何诱导神经元解剖结构的永久性差异的机制,但仍不清楚。表观遗传变化,如 DNA 甲基化,允许环境影响改变长期的基因表达模式,因此可能是雌二醇诱导新生大脑组织的潜在介质。在这里,我们回顾了数据,这些数据表明在性二态性脑区的雌激素受体 α (ERα)、雌激素受体 β (ERβ) 和孕激素受体 (PR) 启动子中,性别和雌二醇诱导的 DNA 甲基化存在差异在整个发育过程中。与 DNA 甲基化为与基因表达直接相关的永久性修饰的总体观点相反,这些数据表明,类固醇激素受体上的甲基化模式在整个生命周期中发生变化,并不一定预示着表达。尽管有必要进一步探讨新生脑中雌二醇诱导的 DNA 甲基化模式改变的机制和意义,但这些结果提供了初步证据,表明表观遗传改变可以响应早期激素暴露而发生,并可能介导新生脑中雌二醇诱导的性别差异组织。

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