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Effects of genetic and early environmental risk factors for depression on serotonin transporter expression and methylation profiles

机译:抑郁的遗传和早期环境危险因素对5-羟色胺转运蛋白表达和甲基化谱的影响

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摘要

The serotonin transporter (SERT) gene-linked polymorphic region (5-HTTLPR) has been implicated in moderating the link between life stress and depression. However, respective molecular pathways of gene–environment (GxE) interaction are largely unknown. Sustained alterations in SERT gene expression profiles, possibly mediated by epigenetic modifications, are a frequent correlate of depression and may thus constitute a putative mediator of GxE interaction. Here, we aimed to investigate joint effects of 5-HTTLPR and self-reported environmental adversity throughout the lifespan (prenatal, early and recent stress/trauma) on in vivo SERT mRNA expression in peripheral blood cells. To further evaluate whether environmentally induced changes in SERT expression are mediated by epigenetic modifications, we analyzed 83 CpG sites within a 799-bp promoter-associated CpG island of the SERT gene using the highly sensitive method of bisulfite pyrosequencing. Participants were 133 healthy young adults. Our findings show that both the 5-HTTLPR S allele and maternal prenatal stress/child maltreatment are associated with reduced in vivo SERT mRNA expression in an additive manner. Remarkably, individuals carrying both the genetic and the environmental risk factors exhibited 32.8% (prenatal stress) and 56.3% (child maltreatment) lower SERT mRNA levels compared with those without any risk factor. Our data further indicated that changes in SERT mRNA levels were unlikely to be mediated by DNA methylation profiles within the SERT CpG island. It is thus conceivable that the persistent changes in SERT expression may in turn relate to altered serotonergic functioning and possibly convey differential disease vulnerability associated with 5-HTTLPR and early adversity.
机译:血清素转运蛋白(SERT)基因连锁的多态性区域(5-HTTLPR)参与减轻生活压力和抑郁之间的联系。但是,基因与环境(GxE)相互作用的各个分子途径尚不清楚。 SERT基因表达谱的持续改变(可能由表观遗传修饰介导)是抑郁症的常见原因,因此可能构成了GxE相互作用的推定介体。在这里,我们旨在调查5-HTTLPR和自我报告的环境逆境在整个生命周期(产前,早期和最近的压力/创伤)对外周血细胞体内SERT mRNA表达的联合影响。若要进一步评估是否由表观遗传修饰介导环境诱导的SERT表达变化,我们使用亚硫酸氢盐焦磷酸测序的高灵敏度方法分析了SERT基因的799 bp启动子相关的CpG岛内的83个CpG位点。参加者为133名健康的年轻人。我们的发现表明,5-HTTLPR S等位基因和母亲产前应激/儿童虐待均以累加方式与体内SERT mRNA表达的降低有关。值得注意的是,与没有遗传因素的人相比,同时具有遗传和环境危险因素的人的SERT mRNA水平降低了32.8%(产前压力)和56.3%(儿童虐待)。我们的数据进一步表明,SERT CpG岛内的DNA甲基化谱不太可能介导SERT mRNA水平的变化。因此可以想象,SERT表达的持续变化可能反过来与血清素能功能的改变有关,并可能传达与5-HTTLPR和早期逆境有关的差异性疾病易感性。

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