首页> 外文期刊>European journal of human genetics: EJHG >Site-specific methylation of placental HSD11B2 gene promoter is related to intrauterine growth restriction
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Site-specific methylation of placental HSD11B2 gene promoter is related to intrauterine growth restriction

机译:胎盘HSD11B2基因启动子的位点特异性甲基化与子宫内生长受限有关

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Intrauterine growth restriction (IUGR) is associated with detrimental effects on neurodevelopmental progress in childhood and higher risk of degenerative diseases in adulthood. Placental 11β-hydroxysteroid dehydrogenase (HSD11B2) is a key gene involved in glucocorticoid metabolism, which in turn seems to be related to fetal growth impairment. As reduction of placental HSD11B2 gene expression has been associated with reduced human fetal growth, and methylation of HSD11B2 gene promoter has been shown to have an important role in HSD11B2 gene repression, we seek to investigate the relationship between IUGR and HSD11B2 gene promoter methylation in human placentas. We found that methylation levels of all studied CpG sites were significantly higher in IUGR newborns than those in controls. Further, methylation levels of the first and the third CpG sites were inversely associated with measures of fetal growth (birth weight and ponderal index). In addition, consistent with the above negative correlation, methylation levels of the first and the third CpG sites were inversely associated with HSD11B2 gene expression. These results together show a link between the site-specific methylation of placental HSD11B2 promoter and the development of IUGR.
机译:宫内生长受限(IUGR)与儿童神经发育进程的有害影响以及成年期发生变性疾病的风险较高相关。胎盘11β-羟类固醇脱氢酶(HSD11B2)是参与糖皮质激素代谢的关键基因,而糖皮质激素代谢又似乎与胎儿生长障碍有关。由于胎盘HSD11B2基因表达的减少与人类胎儿的生长减少有关,并且HSD11B2基因启动子的甲基化已被证明在HSD11B2基因抑制中具有重要作用,因此我们试图研究IUGR与人类HSD11B2基因启动子甲基化之间的关系。胎盘素。我们发现,在IUGR新生儿中,所有研究的CpG位点的甲基化水平均显着高于对照组。此外,第一个和第三个CpG位点的甲基化水平与胎儿生长的指标(出生体重和子宫指数)成反比。另外,与上述负相关性一致,第一和第三CpG位点的甲基化水平与HSD11B2基因表达负相关。这些结果一起显示了胎盘HSD11B2启动子的位点特异性甲基化与IUGR的发展之间的联系。

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