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Phosphorylation of the chromosomal passenger protein Bir1 is required for localization of Ndc10 to the spindle during anaphase and full spindle elongation

机译:在后期和整个纺锤体延伸过程中,Ndc10定位于纺锤体需要染色体过客蛋白Bir1的磷酸化

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摘要

The Saccharomyces cerevisiae inhibitor of apoptosis (IAP) repeat protein Bir1 localizes as a chromosomal passenger. A deletion analysis of Bir1 identified two regions important for function. The C-terminal region is essential for growth, binds Sli15, and is necessary and sufficient for the localization of Bir1 as a chromosomal passenger. The middle region is not essential but is required to localize the inner kinetochore protein Ndc10 to the spindle during anaphase and to the midzone at telophase. In contrast, precise deletion of the highly conserved IAP repeats conferred no phenotype and did not alter the cell cycle delay caused by loss of cohesin. Bir1 is phosphorylated in a cell cycle-dependent manner. Mutation of all nine CDK consensus sites in the middle region of Bir1 significantly decreased the level of phosphorylation and blocked localization of Ndc10 to the spindle at anaphase. Moreover, immunoprecipitation of Ndc10 with Bir1 was dependent on phosphorylation. The loss of Ndc10 from the anaphase spindle prevented elongation of the spindle beyond 7 mu m. We conclude that phosphorylation of the middle region of Bir1 is required to bring Ndc10 to the spindle at anaphase, which is required for full spindle elongation.
机译:酿酒酵母的凋亡抑制剂(IAP)重复蛋白Bir1定位为染色体乘客。 Bir1的删除分析确定了两个重要的功能区域。 C末端区域对于生长必不可少,可与Sli15结合,并且对于将Bir1定位为染色体客体而言是必要且充分的。中间区域不是必不可少的,但在后期阶段将内部动粒蛋白Ndc10定位在纺锤体上,而在末期将其定位在中间区域是必需的。相比之下,高度保守的IAP重复的精确删除不会产生任何表型,并且不会改变由黏附素损失引起的细胞周期延迟。 Bir1以细胞周期依赖性方式被磷酸化。 Bir1中部区域的所有9个CDK共有位点的突变均显着降低了磷酸化水平,并在后期阻止了Ndc10定位于纺锤体。此外,Ndc10与Bir1的免疫沉淀取决于磷酸化。 Ndc10从后期纺锤体中流失,阻止纺锤体伸长超过7微米。我们得出的结论是,需要Bir1中间区域的磷酸化才能将Ndc10在后期带到纺锤体,这是整个纺锤体伸长所必需的。

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