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lncRNA maturation to initiate heterochromatin formation in the nucleolus is required for exit from pluripotency in ESCs

机译:退出胚胎干细胞的多能性需要lncRNA成熟以启动核仁中的异染色质形成

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摘要

The open chromatin of embryonic stem cells (ESCs) condenses into repressive heterochromatin as cells exit the pluripotent state. How the 3D genome organization is orchestrated and implicated in pluripotency and lineage specification is not understood. Here, we find that maturation of the long noncoding RNA (lncRNA) pRNA is required for establishment of heterochromatin at ribosomal RNA genes, the genetic component of nucleoli, and this process is inactivated in pluripotent ESCs. By using mature pRNA to tether heterochromatin at nucleoli of ESCs, we find that localized heterochromatin condensation of ribosomal RNA genes initiates establishment of highly condensed chromatin structures outside of the nucleolus. Moreover, we reveal that formation of such highly condensed, transcriptionally repressed heterochromatin promotes transcriptional activation of differentiation genes and loss of pluripotency. Our findings unravel the nucleolus as an active regulator of chromatin plasticity and pluripotency and challenge current views on heterochromatin regulation and function in ESCs.
机译:当细胞退出多能状态时,胚胎干细胞(ESC)的开放染色质凝结为抑制性异染色质。目前尚不清楚3D基因组的组织方式如何与多能性和谱系规范相关联。在这里,我们发现长非编码RNA(lncRNA)pRNA的成熟是核糖体RNA基因(核仁的遗传成分)建立异染色质所必需的,并且该过程在多能ESC中失活了。通过使用成熟的pRNA将异染色质束缚在ESC的核仁上,我们发现核糖体RNA基因的局部异染色质缩合引发了核仁外部高度浓缩的染色质结构的建立。而且,我们揭示了这种高度浓缩的,转录抑制的异染色质的形成促进了分化基因的转录激活和多能性的丧失。我们的发现揭示了核仁作为染色质可塑性和多能性的活性调节剂,并挑战了目前关于ESC中异染色质调节和功能的观点。

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