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首页> 外文期刊>Journal of cell biology >Condensin complexes regulate mitotic progression and interphase chromatin structure in embryonic stem cells
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Condensin complexes regulate mitotic progression and interphase chromatin structure in embryonic stem cells

机译:凝缩蛋白复合物调节胚胎干细胞中的有丝分裂进程和相间染色质结构

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In an RNA interference screen interrogating regulators of mouse embryonic stem (ES) cell chromatin structure, we previously identified 62 genes required for ES cell viability. Among these 62 genes were Smc2 and - 4 , which are core components of the two mammalian condensin complexes. In this study, we show that for Smc2 and - 4 , as well as an additional 49 of the 62 genes, knockdown (KD) in somatic cells had minimal effects on proliferation or viability. Upon KD, Smc2 and - 4 exhibited two phenotypes that were unique to ES cells and unique among the ES cell–lethal targets: metaphase arrest and greatly enlarged interphase nuclei. Nuclear enlargement in condensin KD ES cells was caused by a defect in chromatin compaction rather than changes in DNA content. The altered compaction coincided with alterations in the abundance of several epigenetic modifications. These data reveal a unique role for condensin complexes in interphase chromatin compaction in ES cells.
机译:在询问小鼠胚胎干(ES)细胞染色质结构的RNA干扰筛选调节剂中,我们先前确定了ES细胞活力所需的62个基因。在这62个基因中,Smc2和-4是这两个哺乳动物的condensin复合体的核心组成部分。在这项研究中,我们表明对于Smc2和-4以及62个基因中的另外49个,体细胞中的敲低(KD)对增殖或活力的影响最小。在KD上,Smc2和-4表现出两种表型,这两种表型是ES细胞所特有的,并且在ES细胞的致死靶标中也很独特:中期停滞和大大扩大的相间核。凝集素KD ES细胞中的核增大是由染色质紧密性缺陷而非DNA含量变化引起的。改变的紧实度与几种表观遗传修饰的丰度变化同时发生。这些数据揭示了凝集素复合物在ES细胞相间染色质压实中的独特作用。

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