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围产期睾酮暴露对小鼠大脑 DNA 甲基组的影响是后期出现的。

The effects of perinatal testosterone exposure on the DNA methylome of the mouse brain are late-emerging.

机构信息

Department of Human Genetics, David Geffen School of Medicine at University of California Los Angeles (UCLA), Los Angeles, CA 90095, USA.

Laboratory of Neuroendocrinology of the Brain Research Institute, UCLA, Los Angeles, CA 90095, USA.

出版信息

Biol Sex Differ. 2014 Jun 13;5:8. doi: 10.1186/2042-6410-5-8. eCollection 2014.

Abstract

BACKGROUND

The biological basis for sex differences in brain function and disease susceptibility is poorly understood. Examining the role of gonadal hormones in brain sexual differentiation may provide important information about sex differences in neural health and development. Permanent masculinization of brain structure, function, and disease is induced by testosterone prenatally in males, but the possible mediation of these effects by long-term changes in the epigenome is poorly understood.

METHODS

We investigated the organizational effects of testosterone on the DNA methylome and transcriptome in two sexually dimorphic forebrain regions-the bed nucleus of the stria terminalis/preoptic area and the striatum. To study the contribution of testosterone to both the establishment and persistence of sex differences in DNA methylation, we performed genome-wide surveys in male, female, and female mice given testosterone on the day of birth. Methylation was assessed during the perinatal window for testosterone's organizational effects and in adulthood.

RESULTS

The short-term effect of testosterone exposure was relatively modest. However, in adult animals the number of genes whose methylation was altered had increased by 20-fold. Furthermore, we found that in adulthood, methylation at a substantial number of sexually dimorphic CpG sites was masculinized in response to neonatal testosterone exposure. Consistent with this, testosterone's effect on gene expression in the striatum was more apparent in adulthood.

CONCLUSION

Taken together, our data imply that the organizational effects of testosterone on the brain methylome and transcriptome are dramatic and late-emerging. Our findings offer important insights into the long-term molecular effects of early-life hormonal exposure.

摘要

背景

大脑功能和疾病易感性的性别差异的生物学基础尚未得到充分理解。研究性腺激素在大脑性分化中的作用可能为神经健康和发育方面的性别差异提供重要信息。雄性在产前被睾丸酮永久地雄性化,导致大脑结构、功能和疾病的雄性化,但长期的表观基因组变化对这些影响的介导作用知之甚少。

方法

我们研究了睾丸酮对两个性别二态性前脑区域——终纹床核/视前区和纹状体——的 DNA 甲基组和转录组的组织效应。为了研究睾丸酮对 DNA 甲基化性别差异的建立和持续的影响,我们在雄性、雌性和出生时给予睾丸酮的雌性小鼠中进行了全基因组调查。在睾丸酮的组织效应的围产期窗口和成年期评估甲基化。

结果

睾丸酮暴露的短期效应相对较小。然而,在成年动物中,其甲基化改变的基因数量增加了 20 倍。此外,我们发现,在成年期,对大量性别二态性 CpG 位点的甲基化在新生期睾丸酮暴露后被雄性化。与这一发现一致的是,睾丸酮对纹状体中基因表达的影响在成年期更为明显。

结论

总之,我们的数据表明,睾丸酮对大脑甲基组和转录组的组织效应是显著的且迟发的。我们的研究结果为早期生命激素暴露的长期分子效应提供了重要的见解。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/39ab/4074311/6c562d045246/2042-6410-5-8-1.jpg

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