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纺锤体检查点蛋白Xmad1将Xmad2募集到未附着的动粒上。

Spindle checkpoint protein Xmad1 recruits Xmad2 to unattached kinetochores.

作者信息

Chen R H, Shevchenko A, Mann M, Murray A W

机构信息

Section of Biochemistry, Molecular and Cell Biology, Cornell University, Ithaca, New York 14853, USA.

出版信息

J Cell Biol. 1998 Oct 19;143(2):283-95. doi: 10.1083/jcb.143.2.283.

Abstract

The spindle checkpoint prevents the metaphase to anaphase transition in cells containing defects in the mitotic spindle or in chromosome attachment to the spindle. When the checkpoint protein Xmad2 is depleted from Xenopus egg extracts, adding Xmad2 to its endogenous concentration fails to restore the checkpoint, suggesting that other checkpoint component(s) were depleted from the extract through their association with Xmad2. Mass spectrometry provided peptide sequences from an 85-kD protein that coimmunoprecipitates with Xmad2 from egg extracts. This information was used to clone XMAD1, which encodes a homologue of the budding yeast (Saccharomyces cerevisiae) checkpoint protein Mad1. Xmad1 is essential for establishing and maintaining the spindle checkpoint in egg extracts. Like Xmad2, Xmad1 localizes to the nuclear envelope and the nucleus during interphase, and to those kinetochores that are not bound to spindle microtubules during mitosis. Adding an anti-Xmad1 antibody to egg extracts inactivates the checkpoint and prevents Xmad2 from localizing to unbound kinetochores. In the presence of excess Xmad2, neither chromosomes nor Xmad1 are required to activate the spindle checkpoint, suggesting that the physiological role of Xmad1 is to recruit Xmad2 to kinetochores that have not bound microtubules.

摘要

纺锤体检查点可防止有丝分裂纺锤体存在缺陷或染色体与纺锤体连接存在缺陷的细胞中发生中期到后期的转变。当爪蟾卵提取物中的检查点蛋白Xmad2被耗尽时,将Xmad2添加至其内源性浓度也无法恢复检查点功能,这表明提取物中的其他检查点成分通过与Xmad2的结合而被耗尽。质谱分析提供了一种与卵提取物中的Xmad2共免疫沉淀的85-kD蛋白的肽序列。该信息被用于克隆XMAD1,它编码芽殖酵母(酿酒酵母)检查点蛋白Mad1的一个同源物。Xmad1对于在卵提取物中建立和维持纺锤体检查点至关重要。与Xmad2一样,Xmad1在间期定位于核膜和细胞核,在有丝分裂期间定位于那些未与纺锤体微管结合的动粒。向卵提取物中添加抗Xmad1抗体可使检查点失活,并阻止Xmad2定位于未结合的动粒。在存在过量Xmad2的情况下,激活纺锤体检查点既不需要染色体也不需要Xmad1,这表明Xmad1的生理作用是将Xmad2招募至未结合微管的动粒。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8d03/2132829/7743ed4b2f04/JCB9807002.f5a.jpg

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