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New-born females show higher stress- and genotype-independent methylation of SLC6A4 than males

机译:新生女性比男性表现出更高的与压力和基因型无关的甲基化SLC6A4

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摘要

BackgroundResearch has demonstrated an association between exposure to early life stress and an increased risk of psychiatric disorders in later life, in particular depression. However, the mechanism through which early life stress contributes to disease development remains unclear. Previous studies have reported an association between early life stress and altered methylation of the serotonin transporter gene (SLC6A4), a key candidate gene for several psychiatric disorders. These differences in methylation are influenced by sex and genetic variation in the SLC6A4-linked polymorphic region (5-HTTLPR). Furthermore, one study indicated that stress during pregnancy may induce methylation changes in SLC6A4 in the newborn. The present study is the first to investigate whether early life stress during pregnancy impacts on SLC6A4 methylation in newborns, taking into account the influence of genetic variation and sex.
机译:背景研究已经证明,暴露于早期生活压力与以后生活中精神疾病(尤其是抑郁症)的风险增加之间存在关联。但是,早期生活压力促进疾病发展的机制仍不清楚。先前的研究报道了早期生活压力与5-羟色胺转运蛋白基因(SLC6A4)的甲基化改变之间的关联,5-羟色胺转运蛋白基因是一些精神疾病的关键候选基因。这些甲基化差异受SLC6A4连接的多态性区域(5-HTTLPR)中的性别和遗传变异影响。此外,一项研究表明,怀孕期间的压力可能会导致新生儿SLC6A4发生甲基化变化。本研究是第一个调查妊娠早期生命压力是否影响新生儿SLC6A4甲基化的方法,同时考虑了遗传变异和性别的影响。

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