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The Role of Placental 11-Beta Hydroxysteroid Dehydrogenase Type 1 and Type 2 Methylation on Gene Expression and Infant Birth Weight

机译:胎盘11-β羟类固醇脱氢酶1型和2型甲基化对基因表达和婴儿出生体重的作用

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摘要

Maternal stress has been linked to infant birth weight outcomes, which itself may be associated with health later in life. The placenta acts as a master regulator for the fetal environment, mediating intrauterine exposures to stress through the activity of genes regulating glucocorticoids, including the 11beta-hydroxysteroid dehydrogenase (HSD11B) type 1 and 2 genes, and so we hypothesized that variation in these genes will be associated with infant birth weight. We investigated DNA methylation levels at six sites across the two genes, as well as mRNA expression for each, and the relationship to infant birth weight. Logistic regressions correcting for potential confounding factors revealed a significant association between methylation at a single CpG site within HSD11B1 and being born large for gestational age. In addition, our analysis identified correlations between methylation and gene expression, including sex-specific transcriptional regulation of HSD11B2. Our work is one of the first comprehensive views of DNA methylation and expression in the placenta for both HSD11B types 1 and 2, linking epigenetic alterations with the regulation of fetal stress and birth weight outcomes.
机译:产妇压力与婴儿出生体重的结果有关,其本身可能与以后的健康有关。胎盘可作为胎儿环境的主要调节剂,通过调节糖皮质激素的基因(包括11β-羟类固醇脱氢酶(HSD11B)1型和2型基因)的活性介导宫内暴露于应激状态,因此我们推测这些基因的变异会与婴儿出生体重有关。我们调查了两个基因中六个位置的DNA甲基化水平,以及每个基因的mRNA表达以及与婴儿出生体重的关系。校正潜在混杂因素的逻辑回归表明,HSD11B1内单个CpG位点的甲基化与出生于胎龄较大的人之间存在显着关联。此外,我们的分析确定了甲基化与基因表达之间的相关性,包括HSD11B2的性别特异性转录调控。我们的工作是HSD11B 1型和2型胎盘DNA甲基化和在胎盘中表达的最全面的见解之一,将表观遗传学改变与胎儿压力和出生体重的调节联系起来。

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