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首页> 外文期刊>Genome research >Dynamics of enhancer chromatin signatures mark the transition from pluripotency to cell specification during embryogenesis
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Dynamics of enhancer chromatin signatures mark the transition from pluripotency to cell specification during embryogenesis

机译:增强子染色质特征的动力学标志着胚胎发生过程中从多能性到细胞规格的转变

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The generation of distinctive cell types that form different tissues and organs requires precise, temporal and spatial control of gene expression. This depends on specific cis-regulatory elements distributed in the noncoding DNA surrounding their target genes. Studies performed on mammalian embryonic stem cells and Drosophila embryos suggest that active enhancers form part of a defined chromatin landscape marked by histone H3 lysine 4 mono-methylation (H3K4me1) and histone H3 lysine 27 acetylation (H3K27ac). Nevertheless, little is known about the dynamics and the potential roles of these marks during vertebrate embryogenesis. Here, we provide genomic maps of H3K4me1/me3 and H3K27ac at four developmental time-points of zebrafish embryogenesis and analyze embryonic enhancer activity. We find that (1) changes in H3K27ac enrichment at enhancers accompany the shift from pluripotency to tissue-specific gene expression, (2) in early embryos, the peaks of H3K27ac enrichment are bound by pluripotent factors such as Nanog, and (3) the degree of evolutionary conservation is higher for enhancers that become marked by H3K27ac at the end of gastrulation, suggesting their implication in the establishment of the most conserved (phylotypic) transcriptome that is known to occur later at the pharyngula stage.
机译:形成不同组织和器官的独特细胞类型的产生需要对基因表达的精确,时间和空间控制。这取决于分布在其靶基因周围的非编码DNA中的特定顺式调控元件。对哺乳动物胚胎干细胞和果蝇胚胎进行的研究表明,活性增强剂形成了以组蛋白H3赖氨酸4单甲基化(H3K4me1)和组蛋白H3赖氨酸27乙酰化(H3K27ac)为特征的染色质景观。然而,关于脊椎动物胚胎发生过程中这些标记的动力学及其潜在作用知之甚少。在这里,我们提供了斑马鱼胚胎发生的四个发育时间点的H3K4me1 / me3和H3K27ac的基因组图,并分析了胚胎增强子的活性。我们发现(1)增强子处H3K27ac富集的变化伴随着从多能性向组织特异性基因表达的转变;(2)在早期胚胎中,H3K27ac富集的峰值受到多能因子如Nanog的束缚,以及(3)对于在胃形成结束时以H3K27ac标记的增强子,进化保守的程度更高,这表明它们与建立最保守的(系统型)转录组有关,已知该转录组将在咽部后期出现。

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