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首页> 外文期刊>Nature Communications >PICH promotes sister chromatid disjunction and co-operates with topoisomerase II in mitosis
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PICH promotes sister chromatid disjunction and co-operates with topoisomerase II in mitosis

机译:PICH可促进姊妹染色单体分离并与拓扑异构酶II共同作用于有丝分裂

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摘要

PICH is a SNF2 family DNA translocase that binds to ultra-fine DNA bridges (UFBs) in mitosis. Numerous roles for PICH have been proposed from protein depletion experiments, but a consensus has failed to emerge. Here, we report that deletion of PICH in avian cells causes chromosome structural abnormalities, and hypersensitivity to an inhibitor of Topoisomerase II (Topo II), ICRF-193. ICRF-193-treated PICH-/- cells undergo sister chromatid non-disjunction in anaphase, and frequently abort cytokinesis. PICH co-localizes with Topo II alpha on UFBs and at the ribosomal DNA locus, and the timely resolution of both structures depends on the ATPase activity of PICH. Purified PICH protein strongly stimulates the catalytic activity of Topo II in vitro. Consistent with this, a human PICH-/- cell line exhibits chromosome instability and chromosome condensation and decatenation defects similar to those of ICRF-193-treated cells. We propose that PICH and Topo II cooperate to prevent chromosome missegregation events in mitosis.
机译:PICH是SNF2家族的DNA转位酶,可与有丝分裂中的超细DNA桥(UFB)结合。已经从蛋白质消耗实验中提出了许多用于PICH的作用,但未能达成共识。在这里,我们报告说,禽细胞中PICH的缺失会导致染色体结构异常,并对拓扑异构酶II(Topo II)抑制剂ICRF-193过敏。经ICRF-193处理的PICH-/-细胞在后期进行姐妹染色单体分离,并经常中止胞质分裂。 PICH与Topo II alpha共同定位在UFB和核糖体DNA基因座上,两种结构的及时解析取决于PICH的ATPase活性。纯化的PICH蛋白在体外强烈刺激Topo II的催化活性。与此相一致,人PICH-/-细胞系表现出与ICRF-193处理过的细胞相似的染色体不稳定性,染色体凝集和脱级缺陷。我们建议PICH和Topo II合作,以防止有丝分裂中的染色体错聚事件。

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