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表观遗传机制参与大脑的性别分化。

Epigenetic mechanisms are involved in sexual differentiation of the brain.

机构信息

Department of Anatomy and Neurobiology, Kyoto Prefectural University of Medicine, Kyoto 602-8566, Japan.

出版信息

Rev Endocr Metab Disord. 2012 Sep;13(3):163-71. doi: 10.1007/s11154-012-9202-z.

Abstract

Sexual differentiation of the brain can be considered as a process during which effects of sex steroid hormones secreted during early development is maintained into adulthood. Epigenetic regulation is emerging as a potentially important mechanism of conveyance of long-lasting effects of the hormonal and environmental milieu in the developing brain. Evidence has accumulated to show that epigenetic regulation is involved in the control of sexual differentiation of the brain. In the preoptic area (POA), which is important for male sexual behavior, histones associated with the estrogen receptor (ER) α and aromatase (Arom) gene promoters are differentially acetylated between the sexes, and two subtypes of histone deacetylase (HDAC2 and 4) are associated with the same promoters at higher frequencies in males in the early postnatal period. Since ERα and Arom are essential genes in masculinization of the brain, these findings suggest that histone deacetylation in the early postnatal period is involved in masculinization of the brain. Indeed, inhibition of HDAC activity in males during this period abrogates brain masculinization: structural sexual dimorphism of the bed nucleus of the stria terminalis is eliminated and expression of male sexual behavior is reduced in adulthood. Previous reports have demonstrated that ERα gene expression in the POA is higher in females during the developmental and pubertal periods and in adulthood, indicating that sexually dimorphic ERα expression that appears in early postnatal development is maintained until adulthood by epigenetic programming. The ERα promoter is also more sparsely methylated in females, with an inverse correlation with ERα expression. In addition to the hormonal effect, the amount of maternal care received during postnatal development has a lasting effect on ERα expression mediated by DNA methylation of its promoter. Taken together, these results suggest that epigenetic mechanisms play a central role in the transduction and maintenance of early hormonal and social cues to organize sexually differentiated brain functions.

摘要

大脑的性别分化可以被认为是一个过程,在此过程中,早期发育过程中分泌的性激素的作用会持续到成年期。表观遗传调控作为传达发育中大脑中激素和环境因素的长期影响的潜在重要机制正在出现。有证据表明,表观遗传调控参与了大脑性别分化的控制。在对雄性性行为很重要的视前区(POA)中,与雌激素受体(ER)α和芳香化酶(Arom)基因启动子相关的组蛋白在性别之间存在差异乙酰化,并且两种类型的组蛋白去乙酰化酶(HDAC2 和 4)在雄性中的同一启动子上的关联频率更高在出生后的早期。由于 ERα 和 Arom 是大脑男性化的必需基因,这些发现表明,出生后早期的组蛋白去乙酰化参与了大脑的男性化。事实上,在此期间抑制雄性的 HDAC 活性会消除大脑的男性化:终纹床核的结构性别二态性被消除,成年期雄性性行为的表达减少。先前的报告表明,在发育和青春期以及成年期,POA 中的 ERα 基因表达在雌性中更高,这表明在早期出生后发育中出现的性别二态性 ERα 表达通过表观遗传编程维持到成年期。ERα 启动子在雌性中也较少甲基化,与 ERα 表达呈负相关。除了激素的影响之外,在出生后发育过程中接受的母亲照顾的数量也通过其启动子的 DNA 甲基化对 ERα 表达产生持久影响。总之,这些结果表明,表观遗传机制在传递和维持早期激素和社会线索方面发挥着核心作用,以组织性别分化的大脑功能。

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