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首页> 外文期刊>Journal of Biophysical and Biochemical Cytology >Aurora A kinase phosphorylates Hec1 to regulate metaphase kinetochore–microtubule dynamics
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Aurora A kinase phosphorylates Hec1 to regulate metaphase kinetochore–microtubule dynamics

机译:极光A激酶磷酸化HEC1调节中期运动学 - 微管动态

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Precise regulation of kinetochore–microtubule attachments is essential for successful chromosome segregation. Central to this regulation is Aurora B kinase, which phosphorylates kinetochore substrates to promote microtubule turnover. A critical target of Aurora B is the N-terminal “tail” domain of Hec1, which is a component of the NDC80 complex, a force-transducing link between kinetochores and microtubules. Although Aurora B is regarded as the “master regulator” of kinetochore–microtubule attachment, other mitotic kinases likely contribute to Hec1 phosphorylation. In this study, we demonstrate that Aurora A kinase regulates kinetochore–microtubule dynamics of metaphase chromosomes, and we identify Hec1 S69, a previously uncharacterized phosphorylation target site in the Hec1 tail, as a critical Aurora A substrate for this regulation. Additionally, we demonstrate that Aurora A kinase associates with inner centromere protein (INCENP) during mitosis and that INCENP is competent to drive accumulation of the kinase to the centromere region of mitotic chromosomes. These findings reveal that both Aurora A and B contribute to kinetochore–microtubule attachment dynamics, and they uncover an unexpected role for Aurora A in late mitosis.
机译:Kinetochore-Microotubule附件的精确调节对于成功的染色体隔离是必不可少的。该调节的核心是极光B激酶,其磷酸化Kinetochore底物以促进微管变换。 Aurora B的临界目标是HEC1的N末端“尾”结构域,其是NDC80复合物的组分,在KINETOCHORE和微管之间的力转换连杆。尽管Aurora B被视为Kinetochore-Microtubule附件的“主调节器”,但是其他有丝分裂激酶可能有助于HEC1磷酸化。在这项研究中,我们证明Aurora激酶调节中期染色体的Kinetochore-MicroTumule动态,并且我们鉴定HEC1 S69,以前的HEC1尾部中的先前没有表征磷酸化靶位点,作为该调节的关键极光底物。另外,我们证明Aurora在有丝分裂期间与内厘米蛋白(INCENCP)的激酶辅助,并且INVENPP能够赋予激酶积累到有丝分裂染色体的CENTROMERE区域。这些发现表明,Aurora A和B都有助于Kinetochore-Microtubule附件动态,并且它们在晚期有丝分裂中揭示了极晕症的意外作用。

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