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Aberrant chromosome morphology in human cells defective for Holliday junction resolution

机译:人类细胞的霍利迪连接解析缺陷的异常染色体形态

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In somatic cells, Holliday junctions can be formed between sister chromatids during the recombinational repair of DNA breaks or after replication fork demise. A variety of processes act upon Holliday junctions to remove them from DNA, in events that are critical for proper chromosome segregation. In human cells, the BLM protein, inactivated in individuals with Bloom's syndrome, acts in combination with topoisomerase IIIα, RMI1 and RMI2 (BTR complex) to promote the dissolution of double Holliday junctions~(1,2). Cells defective for BLM exhibit elevated levels of sister chromatid exchanges (SCEs) and patients with Bloom's syndrome develop a broad spectrum of early-onset cancers caused by chromosome instability~3. MUS81-EME1 (refs 4-7), SLX1-SLX4 (refs 8-11) and GEN1 (refs 12, 13) also process Holliday junctions but, in contrast to the BTR complex, do so by endonucleolytic cleavage. Here we deplete these nucleases from Bloom's syndrome cells to analyse human cells compromised for the known Holliday junction dissolution/resolution pathways. We show that depletion of MUS81 and GEN1, or SLX4 and GEN1, from Bloom's syndrome cells results in severe chromosome abnormalities, such that sister chromatids remain interlinked in a side-by-side arrangement and the chromosomes are elongated and segmented. Our results indicate that normally replicating human cells require Holliday junction processing activities to prevent sister chromatid entanglements and thereby ensure accurate chromosome condensation. This phenotype was not apparent when both MUS81 and SLX4 were depleted from Bloom's syndrome cells, suggesting that GEN1 can compensate for their absence. Additionally, we show that depletion of MUS81 or SLX4 reduces the high frequency of SCEs in Bloom's syndrome cells, indicating that MUS81 and SLX4 promote SCE formation, in events that may ultimately drive the chromosome instabilities that underpin early-onset cancers associated with Bloom's syndrome.
机译:在体细胞中,在DNA断裂的重组修复过程中或复制叉消失后,姐妹染色单体之间可形成霍利迪结。在对正确的染色体分离至关重要的事件中,有多种过程作用于霍利迪结,将其从DNA中去除。在人类细胞中,在患有布卢姆综合症的个体中失活的BLM蛋白与拓扑异构酶IIIα,RMI1和RMI2(BTR复合物)结合,促进霍利迪双连接的溶解[1,2]。具有BLM缺陷的细胞表现出姐妹染色单体交换(SCE)水平升高,患有布鲁姆氏综合症的患者因染色体不稳定性〜3而发展出广泛的早发癌症。 MUS81-EME1(参考文献4-7),SLX1-SLX4(参考文献8-11)和GEN1(参考文献12、13)也处理霍利迪结,但与BTR复合体相反,它通过内切核酸酶裂解。在这里,我们从布卢姆综合症细胞中耗尽这些核酸酶,以分析因已知的霍利迪结溶解/分解途径而受损的人类细胞。我们显示,从布卢姆综合征细胞中耗尽MUS81和GEN1或SLX4和GEN1会导致严重的染色体异常,从而使姐妹染色单体以并排排列的方式保持相互联系,并且染色体被拉长和分割。我们的结果表明,正常复制的人类细胞需要霍利迪连接处理活动,以防止姐妹染色单体纠缠,从而确保准确的染色体凝聚。当MUS81和SLX4都从Bloom综合征细胞中耗尽时,这种表型并不明显,这表明GEN1可以弥补它们的缺失。此外,我们显示MUS81或SLX4的耗竭减少了Bloom综合征细胞中SCE的高频率,这表明MUS81和SLX4促进了SCE的形成,最终可能导致染色体不稳定性加剧了与Bloom综合征相关的早发性癌症。

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  • 来源
    《Nature》 |2011年第7340期|p.642-646|共5页
  • 作者

    Thomas Wechsler; Scott Newman; Stephen C. West;

  • 作者单位

    London Research Institute, Cancer Research UK, Clare Hall Laboratories, South Mimms, Hertfordshire EN6 3LD, UK,Present address:Stanford University School of Medicine, Clark Center, 318 Campus Drive, Stanford, California 94305, USA;

    Department of Pathology, University of Cambridge, Tennis Court Road, Cambridge CB2 1QP, UK;

    London Research Institute, Cancer Research UK, Clare Hall Laboratories, South Mimms, Hertfordshire EN6 3LD, UK;

  • 收录信息 美国《科学引文索引》(SCI);美国《工程索引》(EI);美国《生物学医学文摘》(MEDLINE);美国《化学文摘》(CA);
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  • 正文语种 eng
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  • 入库时间 2022-08-18 02:54:34

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