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Regulatory network decoded from epigenomes of surface ectoderm-derived cell types

机译:从表面外胚层来源的细胞类型的表观基因组解码的调控网络

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Developmental history shapes the epigenome and biological function of differentiated cells. Epigenomic patterns have been broadly attributed to the three embryonic germ layers. Here we investigate how developmental origin influences epigenomes. We compare key epigenomes of cell types derived from surface ectoderm (SE), including keratinocytes and breast luminal and myoepithelial cells, against neural crest-derived melanocytes and mesoderm-derived dermal fibroblasts, to identify SE differentially methylated regions (SE-DMRs). DNA methylomes of neonatal keratinocytes share many more DMRs with adult breast luminal and myoepithelial cells than with melanocytes and fibroblasts from the same neonatal skin. This suggests that SE origin contributes to DNA methylation patterning, while shared skin tissue environment has limited effect on epidermal keratinocytes. Hypomethylated SE-DMRs are in proximity to genes with SE relevant functions. They are also enriched for enhancer- and promoter-associated histone modifications in SE-derived cells, and for binding motifs of transcription factors important in keratinocyte and mammary gland biology. Thus, epigenomic analysis of cell types with common developmental origin reveals an epigenetic signature that underlies a shared gene regulatory network.
机译:发育史决定了分化细胞的表观基因组和生物学功能。表观基因组模式已广泛归因于三个胚芽层。在这里,我们研究发育起源如何影响表观基因组。我们比较了源自表面外胚层(SE)的细胞类型的关键表观基因组,包括角质形成细胞,乳腺腔和肌上皮细胞与神经c衍生的黑素细胞和中胚层衍生的真皮成纤维细胞,以鉴定SE差异甲基化区域(SE-DMRs)。与来自同一新生皮肤的黑素细胞和成纤维细胞相比,新生角质形成细胞的DNA甲基化组与成年乳腔和肌上皮细胞共享更多的DMR。这表明SE起源有助于DNA甲基化模式,而共享的皮肤组织环境对表皮角质形成细胞的作用有限。次甲基化的SE-DMR靠近具有SE相关功能的基因。它们还丰富了SE衍生细胞中与增强子和启动子相关的组蛋白修饰,以及对于角质形成细胞和乳腺生物学重要的转录因子的结合基序。因此,对具有共同发育起源的细胞类型的表观基因组学分析揭示了表观遗传学特征,它是共享基因调控网络的基础。

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