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Bub3的人类同源物是Bub1和一种Mad3/Bub1相关蛋白激酶着丝粒定位所必需的。

The human homologue of Bub3 is required for kinetochore localization of Bub1 and a Mad3/Bub1-related protein kinase.

作者信息

Taylor S S, Ha E, McKeon F

机构信息

Department of Cell Biology, Harvard Medical School, Boston, Massachusetts 02115, USA.

出版信息

J Cell Biol. 1998 Jul 13;142(1):1-11. doi: 10.1083/jcb.142.1.1.

Abstract

A feedback control mechanism, or cell cycle checkpoint, delays the onset of anaphase until all the chromosomes are correctly aligned on the mitotic spindle. Previously, we showed that the murine homologue of Bub1 is not only required for checkpoint response to spindle damage, but also restrains progression through a normal mitosis (Taylor, S.S., and F. McKeon. 1997. Cell. 89:727-735). Here, we describe the identification of a human homologue of Bub3, a 37-kD protein with four WD repeats. Like Bub1, Bub3 localizes to kinetochores before chromosome alignment. In addition, Bub3 and Bub1 interact in mammalian cells. Deletion mapping was used to identify the domain of Bub1 required for binding Bub3. Significantly, this same domain is required for kinetochore localization of Bub1, suggesting that the role of Bub3 is to localize Bub1 to the kinetochore, thereby activating the checkpoint in response to unattached kinetochores. The identification of a human Mad3/Bub1-related protein kinase, hBubR1, which can also bind Bub3 in mammalian cells, is described. Ectopically expressed hBubR1 also localizes to kinetochores during prometaphase, but only when hBub3 is overexpressed. We discuss the implications of the common interaction between Bub1 and hBubR1 with hBub3 for checkpoint control.

摘要

一种反馈控制机制,即细胞周期检查点,会延迟后期的开始,直到所有染色体在有丝分裂纺锤体上正确排列。此前,我们发现Bub1的小鼠同源物不仅是纺锤体损伤检查点反应所必需的,而且还能抑制正常有丝分裂的进程(泰勒,S.S.,和F.麦基翁。1997年。《细胞》。89:727 - 735)。在这里,我们描述了一种人类Bub3同源物的鉴定,它是一种具有四个WD重复序列的37-kD蛋白。与Bub1一样,Bub3在染色体排列之前定位于动粒。此外,Bub3和Bub1在哺乳动物细胞中相互作用。通过缺失作图来鉴定Bub1与Bub3结合所需的结构域。值得注意的是,Bub1定位于动粒也需要这个相同的结构域,这表明Bub3的作用是将Bub1定位于动粒,从而在对未附着的动粒做出反应时激活检查点。本文还描述了一种人类Mad3/Bub1相关蛋白激酶hBubR1的鉴定,它在哺乳动物细胞中也能与Bub3结合。异位表达的hBubR1在前期也定位于动粒,但仅在hBub3过表达时才会如此。我们讨论了Bub1和hBubR1与hBub3之间的共同相互作用对检查点控制的影响。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/da36/2133037/6ba40bbe3982/JCB9803053.f1.jpg

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