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Hec1 and Nuf2 Are Core Components of the Kinetochore Outer Plate Essential for Organizing Microtubule Attachment SitesV⃞

机译:Hec1和Nuf2是线粒体外板的核心组件,对于组织微管附着位点至关重要

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摘要

A major goal in the study of vertebrate mitosis is to identify proteins that create the kinetochore-microtubule attachment site. Attachment sites within the kinetochore outer plate generate microtubule dependent forces for chromosome movement and regulate spindle checkpoint protein assembly at the kinetochore. The Ndc80 complex, comprised of Ndc80 (Hec1), Nuf2, Spc24, and Spc25, is essential for metaphase chromosome alignment and anaphase chromosome segregation. It has also been suggested to have roles in kinetochore microtubule formation, production of kinetochore tension, and the spindle checkpoint. Here we show that Nuf2 and Hec1 localize throughout the outer plate, and not the corona, of the vertebrate kinetochore. They are part of a stable “core” region whose assembly dynamics are distinct from other outer domain spindle checkpoint and motor proteins. Furthermore, Nuf2 and Hec1 are required for formation and/or maintenance of the outer plate structure itself. Fluorescence light microscopy, live cell imaging, and electron microscopy provide quantitative data demonstrating that Nuf2 and Hec1 are essential for normal kinetochore microtubule attachment. Our results indicate that Nuf2 and Hec1 are required for organization of stable microtubule plus-end binding sites in the outer plate that are needed for the sustained poleward forces required for biorientation at kinetochores.
机译:脊椎动物有丝分裂研究的主要目标是鉴定形成动粒-微管附着位点的蛋白质。线粒体外板内的附着位点产生微管依赖性的染色体移动力,并调节线粒体上纺锤体检查点蛋白的组装。 Ndc80复合体,由Ndc80(Hec1),Nuf2,Spc24和Spc25组成,对于中期染色体比对和后期染色体分离至关重要。还建议它在线粒体微管形成,线粒体张力产生和纺锤体检查点中起作用。在这里,我们显示Nuf2和Hec1定位于整个脊椎动物的动粒的外板,而不是日冕。它们是稳定的“核心”区域的一部分,该区域的装配动态不同于其他外域纺锤体检查点和运动蛋白。此外,Nuf2和Hec1对于形成和/或维持外板结构本身是必需的。荧光显微镜,活细胞成像和电子显微镜提供定量数据,证明Nuf2和Hec1对于正常的动粒微管附着至关重要。我们的结果表明,Nuf2和Hec1是在外部板上组织稳定的微管正端结合位点所必需的,而这些位点对于在动植物处进行生物定向所需的持续极向力是必需的。

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