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Spatial regulation of Aurora A activity during mitotic spindle assembly requires RHAMM to correctly localize TPX2

机译:有丝分裂纺锤体组装过程中Aurora A活动的空间调节需要RHAMM正确定位TPX2

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摘要

Construction of a mitotic spindle requires biochemical pathways to assemble spindle microtubules and structural proteins to organize these microtubules into a bipolar array. Through a complex with dynein, the receptor for hyaluronan-mediated motility (RHAMM) cross-links mitotic microtubules to provide structural support, maintain spindle integrity, and correctly orient the mitotic spindle. Here, we locate RHAMM to sites of microtubule assembly at centrosomes and non-centrosome sites near kinetochores and demonstrate that RHAMM is required for the activation of Aurora kinase A. Silencing of RHAMM delays the kinetics of spindle assembly, mislocalizes targeting protein for XKlp2 (TPX2), and attenuates the localized activation of Aurora kinase A with a consequent reduction in mitotic spindle length. The RHAMM–TPX2 complex requires a C-terminal basic leucine zipper in RHAMM and a domain that includes the nuclear localization signal in TPX2. Together, our findings identify RHAMM as a critical regulator for Aurora kinase A signaling and suggest that RHAMM ensures bipolar spindle assembly and mitotic progression through the integration of biochemical and structural pathways.
机译:有丝分裂纺锤体的构建需要生化途径来组装纺锤体微管和结构蛋白,以将这些微管组织成双极阵列。通过与动力蛋白的复合物,透明质酸介导的运动(RHAMM)受体使有丝分裂微管交联,以提供结构支持,维持纺锤体完整性并正确定向有丝分裂纺锤体。在这里,我们将RHAMM定位于中心粒体和靠近动植物的非中心体部位的微管组装位点,并证明RHAMM是激活Aurora激酶A所必需的。沉默RHAMM会延迟纺锤体组装的动力学,将XKlp2(TPX2)的靶向蛋白错位),并减弱Aurora激酶A的局部激活,从而减少有丝分裂纺锤体的长度。 RHAMM–TPX2复合体在RHAMM中需要一个C端基本亮氨酸拉链,并且在TPX2中需要一个包含核定位信号的域。在一起,我们的发现确定RHAMM是Aurora激酶A信号的关键调节剂,并表明RHAMM通过生化和结构途径的整合来确保双极纺锤体组装和有丝分裂进程。

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