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CENP-C is a blueprint for constitutive centromere–associated network assembly within human kinetochores

机译:CENP-C是人类动植物体内组成性着丝粒相关网络组装的蓝图

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摘要

Kinetochores are multisubunit complexes that assemble on centromeres to bind spindle microtubules and promote faithful chromosome segregation during cell division. A 16-subunit complex named the constitutive centromere–associated network (CCAN) creates the centromere–kinetochore interface. CENP-C, a CCAN subunit, is crucial for kinetochore assembly because it links centromeres with the microtubule-binding interface of kinetochores. The role of CENP-C in CCAN organization, on the other hand, had been incompletely understood. In this paper, we combined biochemical reconstitution and cellular investigations to unveil how CENP-C promotes kinetochore targeting of other CCAN subunits. The so-called PEST domain in the N-terminal half of CENP-C interacted directly with the four-subunit CCAN subcomplex CENP-HIKM. We identified crucial determinants of this interaction whose mutation prevented kinetochore localization of CENP-HIKM and of CENP-TW, another CCAN subcomplex. When considered together with previous observations, our data point to CENP-C as a blueprint for kinetochore assembly.
机译:动植物是多亚基复合物,其在着丝粒上组装以结合纺锤体微管并促进细胞分裂过程中忠实的染色体分离。一个由16个亚基组成的复合体,称为本构性着丝粒相关网络(CCAN),创建了着丝粒-动粒体界面。 CENP-C是CCAN的亚基,对于线粒体组装至关重要,因为它将着丝粒与动植物的微管结合界面联系起来。另一方面,CENP-C在CCAN组织中的作用尚未完全了解。在本文中,我们结合了生化重建和细胞研究,揭示了CENP-C如何促进其他CCAN亚基的线粒体靶向。 CENP-C的N末端一半中的所谓PEST结构域与四亚基CCAN亚复合物CENP-HIKM直接相互作用。我们确定了这种相互作用的关键决定因素,其突变阻止了CENP-HIKM和CENP-TW(另一种CCAN亚复合体)的线粒体定位。当与以前的观察结果一起考虑时,我们的数据表明CENP-C是动线组装的蓝图。

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