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IGF2 基因 DNA 甲基化是调节新生儿胎儿生长发育的一个因素。

IGF2 DNA methylation is a modulator of newborn's fetal growth and development.

机构信息

Department of Pediatrics, Chicoutimi Hospital, Chicoutimi, QC, Canada.

出版信息

Epigenetics. 2012 Oct;7(10):1125-32. doi: 10.4161/epi.21855. Epub 2012 Aug 21.

Abstract

The insulin-like growth factor 2 (IGF2) gene, located within a cluster of imprinted genes on chromosome 11p15, encodes a fetal and placental growth factor affecting birth weight. DNA methylation variability at the IGF2 gene locus has been previously reported but its consequences on fetal growth and development are still mostly unknown in normal pediatric population. We collected one hundred placenta biopsies from 50 women with corresponding maternal and cord blood samples and measured anthropometric indices, blood pressure and metabolic phenotypes using standardized procedures. IGF2/H19 DNA methylation and IGF2 circulating levels were assessed using sodium bisulfite pyrosequencing and ELISA, respectively. Placental IGF2 (DMR0 and DMR2) DNA methylation levels were correlated with newborn's fetal growth indices, such as weight, and with maternal IGF2 circulating concentration at the third trimester of pregnancy, whereas H19 (DMR) DNA methylation levels were correlated with IGF2 levels in cord blood. The maternal genotype of a known IGF2/H19 polymorphism (rs2107425) was associated with birth weight. Taken together, we showed that IGF2/H19 epigenotype and genotypes independently account for 31% of the newborn's weight variance. No association was observed with maternal diabetic status, glucose concentrations or prenatal maternal body mass index. This is the first study showing that DNA methylation at the IGF2/H19 genes locus may act as a modulator of IGF2 newborn's fetal growth and development within normal range. IGF2/H19 DNA methylation could represent a cornerstone in linking birth weight and fetal metabolic programming of late onset obesity.

摘要

胰岛素样生长因子 2(IGF2)基因位于染色体 11p15 的一组印迹基因簇内,编码一种胎儿和胎盘生长因子,影响出生体重。先前已经报道了 IGF2 基因座处的 DNA 甲基化变异性,但在正常儿科人群中,其对胎儿生长和发育的影响仍知之甚少。我们从 50 名女性收集了 100 份胎盘活检样本,以及相应的母血和脐血样本,并使用标准化程序测量了人体测量指标、血压和代谢表型。使用亚硫酸氢盐焦磷酸测序和 ELISA 分别评估 IGF2/H19 的 DNA 甲基化和 IGF2 循环水平。胎盘 IGF2(DMR0 和 DMR2)DNA 甲基化水平与新生儿的胎儿生长指数(如体重)以及母亲在妊娠晚期的循环 IGF2 浓度相关,而 H19(DMR)DNA 甲基化水平与脐血中的 IGF2 水平相关。一种已知的 IGF2/H19 多态性(rs2107425)的母体基因型与出生体重相关。综上所述,我们表明 IGF2/H19 表型和基因型独立解释了新生儿体重变异的 31%。未观察到与母体糖尿病状态、葡萄糖浓度或产前母体体重指数相关。这是第一项表明 IGF2/H19 基因座处的 DNA 甲基化可能作为正常范围内 IGF2 新生儿胎儿生长和发育的调节剂的研究。IGF2/H19 DNA 甲基化可能是将出生体重与后期肥胖的胎儿代谢编程联系起来的基石。

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