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A three-step MTOC fragmentation mechanism facilitates bipolar spindle assembly in mouse oocytes.

机译:三步mTOC碎裂机制有利于小鼠卵母细胞中的双极纺锤体组装。

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摘要

Assembly of a bipolar microtubule spindle is essential for accurate chromosome segregation. In somatic cells, spindle bipolarity is determined by the presence of exactly two centrosomes. Remarkably, mammalian oocytes do not contain canonical centrosomes. This study reveals that mouse oocytes assemble a bipolar spindle by fragmenting multiple acentriolar microtubule-organizing centres (MTOCs) into a high number of small MTOCs to be able to then regroup and merge them into two equal spindle poles. We show that MTOCs are fragmented in a three-step process. First, PLK1 triggers a decondensation of the MTOC structure. Second, BicD2-anchored dynein stretches the MTOCs into fragmented ribbons along the nuclear envelope. Third, KIF11 further fragments the MTOCs following nuclear envelope breakdown so that they can be evenly distributed towards the two spindle poles. Failure to fragment MTOCs leads to defects in spindle assembly, which delay chromosome individualization and congression, putting the oocyte at risk of aneuploidy.
机译:双极微管纺锤体的组装对于准确的染色体分离至关重要。在体细胞中,纺锤体双极性由恰好两个中心体的存在决定。值得注意的是,哺乳动物卵母细胞不含规范的中心体。这项研究表明,小鼠卵母细胞通过将多个羊膜小管微管组织中心(MTOC)破碎成大量的小MTOC来组装双极纺锤体,然后能够将它们重组并合并为两个相等的纺锤体极。我们表明,MTOC分为三个步骤。首先,PLK1触发MTOC结构的缩聚。其次,BicD2锚定的动力蛋白将MTOC沿核被膜拉伸成碎片。第三,KIF11在核包膜破裂后进一步使MTOC破碎,从而它们可以均匀地分布在两个主轴上。未能使MTOC片段化会导致纺锤体装配缺陷,从而延迟染色体个体化和聚集,使卵母细胞处于非整倍性的风险中。

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  • 作者

    Clift, D.; Schuh, M.;

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  • 年度 2015
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  • 原文格式 PDF
  • 正文语种 eng
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