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人类纺锤体检查点控制机制的组成部分特异性定位于双着丝粒染色体上的活性着丝粒。

Components of the human spindle checkpoint control mechanism localize specifically to the active centromere on dicentric chromosomes.

作者信息

Saffery R, Irvine D V, Griffiths B, Kalitsis P, Choo K H

机构信息

Murdoch Childrens Research Institute, Royal Children's Hospital, Parkville, Australia.

出版信息

Hum Genet. 2000 Oct;107(4):376-84. doi: 10.1007/s004390000386.

Abstract

The spindle checkpoint control mechanism functions to ensure faithful chromosome segregation by delaying cell division until all chromosomes are correctly oriented on the mitotic spindle. Initially identified in budding yeast, several mammalian spindle checkpoint-associated proteins have recently been identified and partially characterized. These proteins associate with all active human centromeres, including neocentromeres, in the early stages of mitosis prior to the commencement of anaphase. We have examined the status of proteins associated with the checkpoint protein complex (BUB1, BUBR1, BUB3, MAD2), the anaphase-promoting complex (Tsg24, p55CDC), and other proteins associated with mitotic checkpoint control (ERK1, 3F3/2 epitope, hZW10), on a human dicentric chromosome. Each of these proteins was found to specifically associate with only the active centromere, suggesting that only active centromeres participate in the spindle checkpoint. This finding complements previous studies on multicentric chromosomes demonstrating specific association of structural and motor-related centromere proteins with active centromeres, and suggests that centromere inactivation is accompanied by loss of all functionally important centromere proteins.

摘要

纺锤体检查点控制机制的作用是通过延迟细胞分裂,直到所有染色体在有丝分裂纺锤体上正确定向,从而确保染色体的忠实分离。最初在芽殖酵母中发现,最近已经鉴定出几种与哺乳动物纺锤体检查点相关的蛋白质,并对其进行了部分表征。这些蛋白质在有丝分裂后期开始之前的早期阶段,与包括新着丝粒在内的所有活跃人类着丝粒相关联。我们已经研究了与检查点蛋白复合物(BUB1、BUBR1、BUB3、MAD2)、后期促进复合物(Tsg24、p55CDC)以及与有丝分裂检查点控制相关的其他蛋白质(ERK1、3F3/2表位、hZW10)相关的蛋白质在人类双着丝粒染色体上的状态。发现这些蛋白质中的每一种都仅与活跃着丝粒特异性相关联,这表明只有活跃着丝粒参与纺锤体检查点。这一发现补充了先前关于多着丝粒染色体的研究,这些研究表明结构和运动相关的着丝粒蛋白与活跃着丝粒有特异性关联,并表明着丝粒失活伴随着所有功能重要的着丝粒蛋白的丧失。

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