DNA甲基化
DNMT1型
生物
DNA甲基转移酶
表观遗传学
表观基因组
甲基化
甲基转移酶
体育锻炼的表观遗传学
基因组印记
表观遗传学
基因表达调控
亚硫酸氢盐测序
RNA导向的DNA甲基化
分子生物学
遗传学
细胞生物学
基因表达
基因
作者
Boris Novakovic,Nicholas C. Wong,Mandy Sibson,Hong-Kiat Ng,Ruth Morley,Ursula Manuelpillai,Thomas A. Down,Vardhman K. Rakyan,Stephan Beck,Stefan Hiendleder,Claire T. Roberts,Jeffrey M Craig,Richard Saffery
标识
DOI:10.1074/jbc.m109.064956
摘要
The genome of extraembryonic tissue, such as the placenta, is hypomethylated relative to that in somatic tissues. However, the origin and role of this hypomethylation remains unclear. The DNA methyltransferases DNMT1, -3A, and -3B are the primary mediators of the establishment and maintenance of DNA methylation in mammals. In this study, we investigated promoter methylation-mediated epigenetic down-regulation of DNMT genes as a potential regulator of global methylation levels in placental tissue. Although DNMT3A and -3B promoters lack methylation in all somatic and extraembryonic tissues tested, we found specific hypermethylation of the maintenance DNA methyltransferase (DNMT1) gene and found hypomethylation of the DNMT3L gene in full term and first trimester placental tissues. Bisulfite DNA sequencing revealed monoallelic methylation of DNMT1, with no evidence of imprinting (parent of origin effect). In vitro reporter experiments confirmed that DNMT1 promoter methylation attenuates transcriptional activity in trophoblast cells. However, global hypomethylation in the absence of DNMT1 down-regulation is apparent in non-primate placentas and in vitro derived human cytotrophoblast stem cells, suggesting that DNMT1 down-regulation is not an absolute requirement for genomic hypomethylation in all instances. These data represent the first demonstration of methylation-mediated regulation of the DNMT1 gene in any system and demonstrate that the unique epigenome of the human placenta includes down-regulation of DNMT1 with concomitant hypomethylation of the DNMT3L gene. This strongly implicates epigenetic regulation of the DNMT gene family in the establishment of the unique epigenetic profile of extraembryonic tissue in humans.
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