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出生体重与人类胎盘糖皮质激素受体 DNA 启动子甲基化有关。

Birthweight is associated with DNA promoter methylation of the glucocorticoid receptor in human placenta.

机构信息

Department of Pathology and Laboratory Medicine, Brown University, Providence, RI, USA.

出版信息

Epigenetics. 2011 May;6(5):566-72. doi: 10.4161/epi.6.5.15236. Epub 2011 May 1.

Abstract

Birthweight has been associated with a number of health outcomes throughout life. Crucial to proper infant growth and development is the placenta, and alterations to placental gene function may reflect differences in the intrauterine environment which functionally contribute to infant growth and may ultimately affect the child's health. To examine if epigenetic alteration to the glucocorticoid receptor (GR) gene was linked to infant growth, we analyzed 480 human placentas for differential methylation of the GR gene exon 1F and examined how this variation in methylation extent was associated with fetal growth. Multivariable linear regression revealed a significant association (p < 0.0001) between differential methylation of the GR gene and large for gestational age (LGA) status. Our work is one of the first to link infant growth as a measure of the intrauterine environment and epigenetic alterations to the GR and suggests that DNA methylation may be a critical determinant of placental function.

摘要

出生体重与一生中的许多健康结果有关。胎盘对于婴儿的正常生长和发育至关重要,而胎盘基因功能的改变可能反映了宫内环境的差异,这些差异在功能上有助于婴儿的生长,并最终可能影响儿童的健康。为了研究糖皮质激素受体(GR)基因的表观遗传改变是否与婴儿生长有关,我们分析了 480 个人类胎盘中 GR 基因外显子 1F 的差异甲基化,并研究了这种甲基化程度的变化与胎儿生长的关系。多变量线性回归显示,GR 基因的差异甲基化与大于胎龄儿(LGA)状态之间存在显著关联(p<0.0001)。我们的工作首次将婴儿生长作为宫内环境的衡量标准以及对 GR 的表观遗传改变联系起来,并表明 DNA 甲基化可能是胎盘功能的一个关键决定因素。

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