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Generation of bivalent chromatin domains during cell fate decisions

机译:细胞命运决定过程中二价染色质域的生成

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Background In self-renewing, pluripotent cells, bivalent chromatin modification is thought to silence (H3K27me3) lineage control genes while 'poising' (H3K4me3) them for subsequent activation during differentiation, implying an important role for epigenetic modification in directing cell fate decisions. However, rather than representing an equivalently balanced epigenetic mark, the patterns and levels of histone modifications at bivalent genes can vary widely and the criteria for identifying this chromatin signature are poorly defined. Results Here, we initially show how chromatin status alters during lineage commitment and differentiation at a single well characterised bivalent locus. In addition we have determined how chromatin modifications at this locus change with gene expression in both ensemble and single cell analyses. We also show, on a global scale, how mRNA expression may be reflected in the ratio of H3K4me3/H3K27me3. Conclusions While truly 'poised' bivalently modified genes may exist, the original hypothesis that all bivalent genes are epigenetically premarked for subsequent expression might be oversimplistic. In fact, from the data presented in the present work, it is equally possible that many genes that appear to be bivalent in pluripotent and multipotent cells may simply be stochastically expressed at low levels in the process of multilineage priming. Although both situations could be considered to be forms of 'poising', the underlying mechanisms and the associated implications are clearly different.
机译:背景技术在自我更新的多能细胞中,二价染色质修饰被认为可以沉默(H3K27me3)谱系控制基因,而将它们“保持”(H3K4me3)在分化过程中随后激活,这意味着表观遗传修饰在指导细胞命运决定中起着重要作用。然而,不是代表一个等效的平衡表观遗传标记,而是在二价基因上组蛋白修饰的模式和水平可以有很大的不同,并且鉴定该染色质特征的标准定义不清。结果在这里,我们最初显示了在单个特征明确的二价基因座的谱系定型和分化过程中,染色质状态如何变化。此外,我们已经确定在整体和单细胞分析中,该基因座处的染色质修饰如何随基因表达而变化。我们还显示了在全球范围内,mRNA表达如何以H3K4me3 / H3K27me3的比率反映出来。结论虽然可能存在真正的“平衡”的二价修饰基因,但最初的假设(即所有二价基因都被表观遗传标记为后续表达)可能过于简单。实际上,从本研究中提供的数据来看,在多能启动过程中,很可能在多能细胞和多能细胞中似乎是二价的许多基因可以简单地以低水平随机表达。尽管两种情况都可以视为“蓄势待发”的形式,但其潜在机制和相关含义显然不同。

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