首页> 美国卫生研究院文献>The Journal of Biophysical and Biochemical Cytology >The kinetoplastid kinetochore protein KKT4 is an unconventional microtubule tip–coupling protein
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The kinetoplastid kinetochore protein KKT4 is an unconventional microtubule tip–coupling protein

机译:动素体动粒蛋白KKT4是非常规的微管末端偶联蛋白

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摘要

Kinetochores are multiprotein machines that drive chromosome segregation by maintaining persistent, load-bearing linkages between chromosomes and dynamic microtubule tips. Kinetochores in commonly studied eukaryotes bind microtubules through widely conserved components like the Ndc80 complex. However, in evolutionarily divergent kinetoplastid species such as Trypanosoma brucei, which causes sleeping sickness, the kinetochores assemble from a unique set of proteins lacking homology to any known microtubule-binding domains. Here, we show that the T. brucei kinetochore protein KKT4 binds directly to microtubules and maintains load-bearing attachments to both growing and shortening microtubule tips. The protein localizes both to kinetochores and to spindle microtubules in vivo, and its depletion causes defects in chromosome segregation. We define a microtubule-binding domain within KKT4 and identify several charged residues important for its microtubule-binding activity. Thus, despite its lack of significant similarity to other known microtubule-binding proteins, KKT4 has key functions required for driving chromosome segregation. We propose that it represents a primary element of the kinetochore–microtubule interface in kinetoplastids.
机译:动植物是一种多蛋白机器,通过维持染色体与动态微管尖端之间的持久,承重联系来驱动染色体分离。常用的真核生物中的动植物通过诸如Ndc80复合物之类的广泛保守的成分结合微管。然而,在引起睡眠病的进化上不同的动植物体物种中,例如布鲁氏锥虫,动植物由一组独特的蛋白质组装而成,这些蛋白质与任何已知的微管结合域都缺乏同源性。在这里,我们显示了布鲁氏球菌的线粒体蛋白KKT4直接与微管结合,并保持对增长和缩短的微管尖端的负载附着。该蛋白在体内既定位于动植物,又定位于纺锤体微管,并且其消耗导致染色体分离的缺陷。我们在KKT4中定义了一个微管结合域,并确定了对其微管结合活性重要的几个带电残基。因此,尽管KKT4与其他已知的微管结合蛋白缺乏显着相似性,但它具有驱动染色体分离所需的关键功能。我们建议它代表动质体中动线体-微管界面的主要元素。

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