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Brain feminization requires active repression of masculinization via DNA methylation

机译:脑部女性化需要通过DNA甲基化来积极抑制男性化

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The developing mammalian brain is destined for a female phenotype unless exposed to gonadal hormones during a perinatal sensitive period. It has been assumed that the undifferentiated brain is masculinized by direct induction of transcription by ligand-activated nuclear steroid receptors. We found that a primary effect of gonadal steroids in the highly sexually dimorphic preoptic area (POA) is to reduce activity of DNA methyltransferase (Dnmt) enzymes, thereby decreasing DNA methylation and releasing masculinizing genes from epigenetic repression. Pharmacological inhibition of Dnmts mimicked gonadal steroids, resulting in masculinized neuronal markers and male sexual behavior in female rats. Conditional knockout of the de novo Dnmt isoform, Dnmt3a, also masculinized sexual behavior in female mice. RNA sequencing revealed gene and isoform variants modulated by methylation that may underlie the divergent reproductive behaviors of males versus females. Our data show that brain feminization is maintained by the active suppression of masculinization via DNA methylation.
机译:发育中的哺乳动物大脑注定具有女性表型,除非在围产期敏感期内暴露于性腺激素。假定未分化的大脑是通过配体激活的核甾体受体直接诱导转录而被男性化的。我们发现,在高度性二态性视前区(POA)中,性腺类固醇的主要作用是降低DNA甲基转移酶(Dnmt)酶的活性,从而降低DNA甲基化并从表观遗传抑制中释放男性化基因。 Dnmts模拟的性腺类固醇的药理抑制作用,导致雌性大鼠中男性化的神经元标记和男性性行为。从头敲除Dnmt同工型Dnmt3a也会使雌性小鼠的性行为男性化。 RNA测序揭示了甲基化调控的基因和同工型变异,可能是男性与女性生殖行为不同的基础。我们的数据表明,通过DNA甲基化积极抑制男性化可以保持大脑女性化。

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