Literature DB >> 18640974

Phosphorylation of HsMis13 by Aurora B kinase is essential for assembly of functional kinetochore.

Yong Yang1, Fang Wu, Tarsha Ward, Feng Yan, Quan Wu, Zhaoyang Wang, Tanisha McGlothen, Wei Peng, Tianpa You, Mingkuan Sun, Taixing Cui, Renming Hu, Zhen Dou, Jingde Zhu, Wei Xie, Zihe Rao, Xia Ding, Xuebiao Yao.   

Abstract

Chromosome movements in mitosis are orchestrated by dynamic interactions between spindle microtubules and the kinetochore, a multiprotein complex assembled onto centromeric DNA of the chromosome. Here we show that phosphorylation of human HsMis13 by Aurora B kinase is required for functional kinetochore assembly in HeLa cells. Aurora B interacts with HsMis13 in vitro and in vivo. HsMis13 is a cognate substrate of Aurora B, and the phosphorylation sites were mapped to Ser-100 and Ser-109. Suppression of Aurora B kinase by either small interfering RNA or chemical inhibitors abrogates the localization of HsMis13 but not HsMis12 to the kinetochore. In addition, non-phosphorylatable but not wild type and phospho-mimicking HsMis13 failed to localize to the kinetochore, demonstrating the requirement of phosphorylation by Aurora B for the assembly of HsMis13 to kinetochore. In fact, localization of HsMis13 to the kinetochore is spatiotemporally regulated by Aurora B kinase, which is essential for recruiting outer kinetochore components such as Ndc80 components and CENP-E for functional kinetochore assembly. Importantly, phospho-mimicking mutant HsMis13 restores the assembly of CENP-E to the kinetochore, and tension developed across the sister kinetochores in Aurora B-inhibited cells. Thus, we reason that HsMis13 phosphorylation by Aurora B is required for organizing a stable bi-oriented microtubule kinetochore attachment that is essential for faithful chromosome segregation in mitosis.

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Year:  2008        PMID: 18640974      PMCID: PMC2546542          DOI: 10.1074/jbc.M804207200

Source DB:  PubMed          Journal:  J Biol Chem        ISSN: 0021-9258            Impact factor:   5.157


  30 in total

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  43 in total

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Review 2.  Reconstituting the kinetochore–microtubule interface: what, why, and how.

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6.  Distinct Roles of the Chromosomal Passenger Complex in the Detection of and Response to Errors in Kinetochore-Microtubule Attachment.

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Review 7.  Connecting the microtubule attachment status of each kinetochore to cell cycle arrest through the spindle assembly checkpoint.

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8.  Hsp90-Sgt1 and Skp1 target human Mis12 complexes to ensure efficient formation of kinetochore-microtubule binding sites.

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10.  MiCroKit 3.0: an integrated database of midbody, centrosome and kinetochore.

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