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Fta2, an Essential Fission Yeast Kinetochore Component, Interacts Closely with the Conserved Mal2 Protein

机译:Fta2,必不可少的裂变酵母线粒体组件,与保守的Mal2蛋白紧密相互作用

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摘要

The fission yeast multiprotein-component Sim4 complex plays a fundamental role in the assembly of a functional kinetochore. It affects centromere association of the histone H3 variant CENP-A as well as kinetochore association of the DASH complex. Here, multicopy suppressor analysis of a mutant version of the Sim4 complex component Mal2 identified the essential Fta2 kinetochore protein, which is required for bipolar chromosome attachment. Kinetochore localization of Mal2 and Fta2 depends on each other, and overexpression of one protein can rescue the phenotype of the mutant version of the other protein. fta2 mal2 double mutants were inviable, implying that the two proteins have an overlapping function. This close interaction with Fta2 is not shared by other Sim4 complex components, indicating the existence of functional subgroups within this complex. The Sim4 complex seems to be assembled in a hierarchical way, because Fta2 is localized correctly in a sim4 mutant. However, Fta2 kinetochore localization is reduced in a spc7 mutant. Spc7, a suppressor of the EB1 family member Mal3, is part of the conserved Ndc80–MIND–Spc7 kinetochore complex.
机译:裂变酵母多蛋白成分Sim4复合物在功能性动粒的组装中起着基本作用。它影响组蛋白H3变体CENP-A的着丝粒结合以及DASH复合物的动粒结合。在这里,Sim4复杂成分Mal2的突变体版本的多拷贝抑制器分析确定了必需的Fta2线粒体蛋白,这是双极染色体附着所必需的。 Mal2和Fta2的线粒体定位相互依赖,并且一种蛋白质的过度表达可以挽救另一种蛋白质的突变形式的表型。 fta2 mal2双突变体是不可行的,表明这两种蛋白具有重叠功能。与Sim2复杂组件之间没有共享与Fta2的紧密交互,这表明该复杂组件中存在功能性亚组。 Sim4复合体似乎是以分层方式组装的,因为Fta2正确定位在sim4突变体中。但是,在spc7突变体中Fta2线粒体的定位降低了。 Spc7是EB1家族成员Mal3的抑制剂,是Ndc80–MIND–Spc7线粒体保守分子的一部分。

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