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Developmental fate and cellular maturity encoded in human regulatory DNA landscapes

机译:人类调节性DNA格局编码的发育命运和细胞成熟度

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Cellular-state information between generations of developing cells may be propagated via regulatory regions. We report consistent patterns of gain and loss of DNase I-hypersensitive sites (DHSs) as cells progress from embryonic stem cells (ESCs) to terminal fates. DHS patterns alone convey rich information about cell fate and lineage relationships distinct from information conveyed by gene expression. Developing cells share a proportion of their DHS landscapes with ESCs; that proportion decreases continuously in each cell type as differentiation progresses, providing a quantitative benchmark of developmental maturity. Developmentally stable DHSs densely encode binding sites for transcription factors involved in autoregulatory feedback circuits. In contrast to normal cells, cancer cells extensively reactivate silenced ESC DHSs and those from developmental programs external to the cell lineage from which the malignancy derives. Our results point to changes in regulatory DNA landscapes as quantitative indicators of cell-fate transitions, lineage relationships, and dysfunction. PaperClip
机译:发育细胞世代之间的细胞状态信息可通过调节区传播。我们报告随着细胞从胚胎干细胞(ESC)到最终命运的进展,DNase I超敏性位点(DHSs)的获得和失去的一致性模式。 DHS模式仅传达有关细胞命运和谱系关系的丰富信息,而不同于基因表达所传达的信息。发育中的细胞与胚胎干细胞共享其DHS格局的一部分;随着分化的进展,每种细胞类型的比例不断降低,为发育成熟提供了定量基准。发展稳定的DHS紧密编码与自动调节反馈电路有关的转录因子的结合位点。与正常细胞相反,癌细胞会广泛激活沉默的ESC DHS和来自恶性起源于细胞谱系之外的发育程序的癌细胞。我们的研究结果表明,调节性DNA格局的变化是细胞命运转变,谱系关系和功能障碍的定量指标。回形针

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