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Klf4 organizes long-range chromosomal interactions with the oct4 locus in reprogramming and pluripotency.

机译:Klf4在重编程和多能性方面与oct4基因座组织了远程染色体相互作用。

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Epigenetic mechanisms underlying somatic reprogramming have been extensively studied, but little is?known about the nuclear architecture of pluripotent stem cells (PSCs). Using circular chromosome?conformation capture with high-throughput sequencing (4C-seq) and fluorescence in?situ hybridization (FISH), we identified chromosomal regions that colocalize frequently with the Oct4 locus in PSCs. These PSC-specific long-range interactions are established prior to transcriptional activation of endogenous Oct4 during reprogramming to induced PSCs and are facilitated by Klf4-mediated recruitment of cohesin. Depletion of Klf4 leads to unloading of cohesin at the Oct4 enhancer and disrupts long-range interactions prior to loss of Oct4 transcription and subsequent PSC differentiation, suggesting a causative role for Klf4 in facilitating long-range interactions independent of its transcriptional activity. Taken together, our results delineate the basic nuclear organization at the Oct4 locus in PSCs and suggest a functional role for Klf4-mediated higher-order chromatin structure in maintaining and inducing pluripotency.
机译:体细胞重编程基础的表观遗传机制已被广泛研究,但对多能干细胞(PSCs)的核结构了解甚少。利用高通量测序(4C-seq)和荧光原位杂交(FISH)的环状染色体构象捕获,我们鉴定了在PSC中经常与Oct4基因座共定位的染色体区域。这些PSC特异的远程相互作用是在重编程为诱导的PSC期间内源性Oct4的转录激活之前建立的,并通过Klf4介导的粘着素募集而得以促进。 Klf4的耗尽会导致Oct4增强子上黏附素的卸载,并破坏长距离的相互作用,然后再失去Oct4转录和随后的PSC分化,这表明Klf4在促进长距离相互作用中起着独立于其转录活性的作用。综上所述,我们的研究结果描绘了PSC中Oct4位点的基本核组织,并暗示了Klf4介导的高级染色质结构在维持和诱导多能性中的功能性作用。

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