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Epigenomic profiling indicates a role for DNA methylation in early postnatal liver development

机译:表观基因组分析表明DNA甲基化在出生后早期肝脏发育中的作用

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The question of whether DNA methylation contributes to the stabilization of gene expression patterns in differentiated mammalian tissues remains controversial. Using genome-wide methylation profiling, we screened 3757 gene promoters for changes in methylation during postnatal liver development to test the hypothesis that developmental changes in methylation and expression are temporally correlated. We identified 31 genes that gained methylation and 111 that lost methylation from embryonic day 17.5 to postnatal day 21. Promoters undergoing methylation changes in postnatal liver tended not to be associated with CpG islands. At most genes studied, developmental changes in promoter methylation were associated with expression changes, suggesting both that transcriptional inactivity attracts de novo methylation, and that transcriptional activity can override DNA methylation and successively induce developmental hypomethylation. These in vivo data clearly indicate a role for DNA methylation in mammalian differentiation, and provide the novel insight that critical windows in mammalian developmental epigenetics extend well beyond early embryonic development.
机译:DNA甲基化是否有助于稳定分化哺乳动物组织中基因表达模式的问题仍然存在争议。使用全基因组甲基化分析,我们筛查了3757个基因启动子在产后肝脏发育过程中甲基化的变化,以检验甲基化和表达的发育变化在时间上相关的假设。我们从胚胎第17.5天到出生后第21天,鉴定了31个获得甲基化的基因和111个失去甲基化的基因。在出生后肝脏中发生甲基化变化的启动子往往与CpG岛无关。在大多数研究的基因中,启动子甲基化的发育变化与表达变化相关,这表明转录无活性吸引了从头甲基化,并且转录活性可以覆盖DNA甲基化并依次诱导发育性低甲基化。这些体内数据清楚地表明了DNA甲基化在哺乳动物分化中的作用,并提供了新的见解,即哺乳动物发育表观遗传学中的关键窗口远远超出了早期胚胎发育。

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