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Aurora A activation in mitosis promoted by BuGZ

机译:极光激活促进发病率促进的bugz

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Protein phase separation or coacervation has emerged as a potential mechanism to regulate biological functions. We have shown that coacervation of a mostly unstructured protein, BuGZ, promotes assembly of spindle and its matrix. BuGZ in the spindle matrix binds and concentrates tubulin to promote microtubule (MT) assembly. It remains unclear, however, whether BuGZ could regulate additional proteins to promote spindle assembly. In this study, we report that BuGZ promotes Aurora A (AurA) activation in vitro. Depletion of BuGZ in cells reduces the amount of phosphorylated AurA on spindle MTs. BuGZ also enhances MCAK phosphorylation. The two zinc fingers in BuGZ directly bind to the kinase domain of AurA, which allows AurA to incorporate into the coacervates formed by BuGZ in vitro. Importantly, mutant BuGZ that disrupts the coacervation activity in vitro fails to promote AurA phosphorylation in Xenopus laevis egg extracts. These results suggest that BuGZ coacervation promotes AurA activation in mitosis.
机译:蛋白质相分离或凝聚物作为调节生物学功能的潜在机制。我们已经表明,剪切主要是非结构化的蛋白质,BUGZ,促进主轴的组装及其基质。纺织矩阵中的BUGZ结合并浓缩管蛋白以促进微管(MT)组件。然而,它仍然尚不清楚,虫子是否可以调节额外的蛋白质以促进主轴组件。在这项研究中,我们报告了Bugz在体外促进极光A(Aura)激活。在细胞中的枯竭降低了主轴MTS上的磷酸化光晕的量。 BUGZ还增强了MCAK磷酸化。 Bugz中的两个锌手指直接与Aura的激酶结构域结合,这使得光环掺入由Bugz体外形成的凝聚体。重要的是,破坏体外凝聚活性的突变虫虫未能促进异戊夫斯蛋蛋提取物中的光环磷酸化。这些结果表明,Bugz CoAceration促进了有丝分裂中的Aura活化。

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