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Microtubule sliding activity of a kinesin-8 promotes spindle assembly and spindle length control

机译:kinesin-8的微管滑动活动可促进主轴组装和主轴长度控制

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摘要

Molecular motors play critical roles in the formation of mitotic spindles, either through controlling the stability of individual microtubules, or by cross-linking and sliding microtubule arrays. Kinesin-8 motors are best known for their regulatory roles in controlling microtubule dynamics. They contain microtubule-destabilizing activities, and restrict spindle length in a wide variety of cell types and organisms. Here, we report for the first time on an anti-parallel microtubule-sliding activity of the budding yeast kinesin-8, Kip3. The in vivo importance of this sliding activity was established through the identification of complementary Kip3 mutants that separate the sliding activity and microtubule destabilizing activity. In conjunction with kinesin-5/Cin8, the sliding activity of Kip3 promotes bipolar spindle assembly and the maintenance of genome stability. We propose a “slide-disassemble” model where Kip3’s sliding and destabilizing activity balance during pre-anaphase. This facilitates normal spindle assembly. However, Kip3’s destabilizing activity dominates in late anaphase, inhibiting spindle elongation and ultimately promoting spindle disassembly.
机译:分子马达通过控制单个微管的稳定性或通过交联和滑动微管阵列在有丝分裂纺锤体的形成中起关键作用。 Kinesin-8电动机以其在控制微管动力学方面的调节作用而闻名。它们具有破坏微管的活性,并限制多种细胞类型和生物体中的纺锤体长度。在这里,我们首次报告了芽孢酵母驱动蛋白8,Kip3的抗平行微管滑动活性。通过鉴定分离滑动活性和微管去稳定活性的互补Kip3突变体,确立了这种滑动活性的体内重要性。与kinesin-5 / Cin8结合,Kip3的滑动活性促进了双极纺锤体的组装和基因组稳定性的维持。我们提出了一种“滑动拆卸”模型,该模型可以在后期前Kip3的滑动和破坏活动平衡。这有助于正常的主轴组装。但是,Kip3的去稳定活性在后期后期占主导地位,从而抑制了主轴的伸长并最终促进了主轴的拆卸。

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