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裂殖酵母转化酸性卷曲螺旋相关蛋白Mia1p/Alp7p是在核膜处形成和维持持久性微管组织中心所必需的。

The fission yeast transforming acidic coiled coil-related protein Mia1p/Alp7p is required for formation and maintenance of persistent microtubule-organizing centers at the nuclear envelope.

作者信息

Zheng Liling, Schwartz Cindi, Wee Liangmeng, Oliferenko Snezhana

机构信息

Cell Dynamics Group, Temasek Life Sciences Laboratory, 117604 Singapore, Singapore.

出版信息

Mol Biol Cell. 2006 May;17(5):2212-22. doi: 10.1091/mbc.e05-08-0811. Epub 2006 Feb 15.

Abstract

Microtubule-organizing centers (MTOCs) concentrate microtubule nucleation, attachment and bundling factors and thus restrict formation of microtubule arrays in spatial and temporal manner. How MTOCs occur remains an exciting question in cell biology. Here, we show that the transforming acidic coiled coil-related protein Mia1p/Alp7p functions in emergence of large MTOCs in interphase fission yeast cells. We found that Mia1p was a microtubule-binding protein that preferentially localized to the minus ends of microtubules and was associated with the sites of microtubule attachment to the nuclear envelope. Cells lacking Mia1p exhibited less microtubule bundles. Microtubules could be nucleated and bundled but were frequently released from the nucleation sites in mia1delta cells. Mia1p was required for stability of microtubule bundles and persistent use of nucleation sites both in interphase and postanaphase array dynamics. The gamma-tubulin-rich material was not organized in large perinuclear or microtubule-associated structures in mia1delta cells. Interestingly, absence of microtubules in dividing wild-type cells prevented appearance of large gamma-tubulin-rich MTOC structures in daughters. When microtubule polymerization was allowed, MTOCs were efficiently assembled de novo. We propose a model where MTOC emergence is a self-organizing process requiring the continuous association of microtubules with nucleation sites.

摘要

微管组织中心(MTOCs)集中了微管成核、附着和捆绑因子,从而以空间和时间方式限制微管阵列的形成。MTOCs如何出现仍然是细胞生物学中一个令人兴奋的问题。在这里,我们表明,转化酸性卷曲螺旋相关蛋白Mia1p/Alp7p在间期裂殖酵母细胞中大型MTOCs的出现中发挥作用。我们发现Mia1p是一种微管结合蛋白,优先定位于微管的负端,并与微管附着于核膜的位点相关。缺乏Mia1p的细胞表现出较少的微管束。微管可以成核和捆绑,但在mia1delta细胞中经常从成核位点释放。Mia1p对于微管束的稳定性以及在间期和后期阵列动态中持续使用成核位点都是必需的。在mia1delta细胞中,富含γ-微管蛋白的物质没有组织成大型的核周或微管相关结构。有趣的是,在分裂的野生型细胞中缺乏微管会阻止子代细胞中出现大型富含γ-微管蛋白的MTOC结构。当允许微管聚合时,MTOCs能够有效地从头组装。我们提出了一个模型,其中MTOC的出现是一个自组织过程,需要微管与成核位点持续关联。

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