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凝聚素是脊椎动物有丝分裂染色体非组蛋白组装和结构完整性所必需的。

Condensin is required for nonhistone protein assembly and structural integrity of vertebrate mitotic chromosomes.

作者信息

Hudson Damien F, Vagnarelli Paola, Gassmann Reto, Earnshaw William C

机构信息

Wellcome Trust Centre for Cell Biology, Institute of Cell, University of Edinburgh, Swann Building, King's Buildings, Mayfield Road, EH9 3JR, Edinburgh, United Kingdom.

出版信息

Dev Cell. 2003 Aug;5(2):323-36. doi: 10.1016/s1534-5807(03)00199-0.

Abstract

The dramatic condensation of chromosomes that occurs during mitosis is widely thought to be largely controlled by a protein complex termed condensin. Here, we describe a conditional knockout of the condensin subunit ScII/SMC2 in chicken DT40 cells. In cells lacking this condensin subunit, chromosome condensation is delayed, but ultimately reaches near-normal levels. However, these chromosomes are structurally compromised. Kinetochores appear normal, but the localization of nonhistone proteins such as topoisomerase II and INCENP is aberrant. Both proteins also fail to partition into the chromosome scaffold fraction, which appears to be largely missing in the absence of condensin. Furthermore, the chromosomes lack structural integrity, as defined by an assay that tests the stability of the chromosomal higher-order structure. Thus, a major function of condensin is to promote the correct association of nonhistone proteins with mitotic chromosomes, and this is essential for establishment of a robust chromosome structure.

摘要

人们普遍认为,有丝分裂过程中发生的染色体剧烈浓缩在很大程度上受一种名为凝聚素的蛋白质复合体控制。在此,我们描述了鸡DT40细胞中凝聚素亚基ScII/SMC2的条件性敲除。在缺乏这种凝聚素亚基的细胞中,染色体浓缩延迟,但最终接近正常水平。然而,这些染色体在结构上存在缺陷。动粒看起来正常,但诸如拓扑异构酶II和染色体乘客蛋白(INCENP)等非组蛋白的定位异常。这两种蛋白质也无法分配到染色体支架部分,在缺乏凝聚素的情况下,染色体支架部分似乎基本缺失。此外,根据一项测试染色体高级结构稳定性的实验,这些染色体缺乏结构完整性。因此,凝聚素的一个主要功能是促进非组蛋白与有丝分裂染色体的正确结合,而这对于建立稳健的染色体结构至关重要。

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