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极光 B 和 14-3-3 共同调节细胞分裂过程中中心纺锤体的聚集。

Aurora B and 14-3-3 coordinately regulate clustering of centralspindlin during cytokinesis.

机构信息

The Wellcome Trust/Cancer Research UK Gurdon Institute, University of Cambridge, Tennis Court Road, Cambridge CB2 1QN, UK.

出版信息

Curr Biol. 2010 May 25;20(10):927-33. doi: 10.1016/j.cub.2010.03.055. Epub 2010 May 6.

Abstract

Centralspindlin is essential for the formation of microtubule bundle structures and the equatorial recruitment of factors critical for cytokinesis. Stable accumulation of centralspindlin at the spindle midzone requires its multimerization into clusters and Aurora B kinase activity, which peaks at the central spindle during anaphase. Although Aurora B phosphorylates centralspindlin directly, how this regulates centralspindlin localization is unknown. Here we identify a novel regulatory mechanism by which Aurora B enables centralspindlin to accumulate stably at the spindle midzone. We show that 14-3-3 protein binds centralspindlin when the kinesin-6 component MKLP1 is phosphorylated at S710. 14-3-3 prevents centralspindlin from clustering in vitro, and an MKLP1 mutant that is unable to bind 14-3-3 forms aberrant clusters in vivo. Interestingly, 14-3-3 binding is inhibited by phosphorylation of S708, a known Aurora B target site that lies within the motif bound by 14-3-3. S708 phosphorylation is required for MKLP1 to stably localize to the central spindle, but it is dispensable in an MKLP1 mutant that does not bind 14-3-3. We propose that 14-3-3 serves as a global inhibitor of centralspindlin that allows Aurora B to locally activate clustering and the stable accumulation of centralspindlin between segregating chromosomes.

摘要

中心纺锤体对于微管束结构的形成和细胞分裂赤道区关键因子的募集是必不可少的。中心纺锤体在纺锤体中间区的稳定积累需要其多聚化为簇,并需要 Aurora B 激酶活性,该活性在后期达到顶峰。尽管 Aurora B 直接磷酸化中心纺锤体,但这种磷酸化如何调节中心纺锤体的定位尚不清楚。在这里,我们确定了一种新的调节机制,通过该机制,Aurora B 能够使中心纺锤体稳定地积累在纺锤体中间区。我们表明,当驱动蛋白-6 成分 MKLP1 在 S710 处被磷酸化时,14-3-3 蛋白与中心纺锤体结合。14-3-3 阻止中心纺锤体在体外聚集,并且无法与 14-3-3 结合的 MKLP1 突变体在体内形成异常聚集。有趣的是,S708 的磷酸化抑制了 14-3-3 的结合,S708 是一个已知的 Aurora B 靶位,位于与 14-3-3 结合的基序内。S708 磷酸化对于 MKLP1 稳定定位于中心纺锤体是必需的,但在不与 14-3-3 结合的 MKLP1 突变体中是可有可无的。我们提出,14-3-3 作为中心纺锤体的全局抑制剂,允许 Aurora B 在分离染色体之间局部激活聚集和中心纺锤体的稳定积累。

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