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Fission yeast ch-TOG/XMAP215 homologue Alp14 connects mitotic spindles with the kinetochore and is a component of the Mad2-dependent spindle checkpoint

机译:裂变酵母ch-TOG / XMAP215同系物Alp14将有丝分裂纺锤体与动粒体连接起来是Mad2依赖性纺锤体检查点的组成部分

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摘要

The TOG/XMAP215-related proteins play a role in microtubule dynamics at its plus end. Fission yeast Alp14, a newly identified TOG/XMAP215 family protein, is essential for proper chromosome segregation in concert with a second homologue Dis1. We show that the alp14 mutant fails to progress towards normal bipolar spindle formation. Intriguingly, Alp14 itself is a component of the Mad2-dependent spindle checkpoint cascade, as upon addition of microtubule-destabilizing drugs the alp14 mutant is incapable of maintaining high H1 kinase activity, which results in securin destruction and premature chromosome separation. Live imaging of Alp14–green fluorescent protein shows that during mitosis, Alp14 is associated with the peripheral region of the kinetochores as well as with the spindle poles. This is supported by ChIP (chromatin immunoprecipitation) and overlapping localization with the kinetochore marker Mis6. An intact spindle is required for Alp14 localization to the kinetochore periphery, but not to the poles. These results indicate that the TOG/XMAP215 family may play a central role as a bridge between the kinetochores and the plus end of pole to chromosome microtubules.
机译:TOG / XMAP215相关蛋白在其正向末端在微管动力学中起作用。裂变酵母Alp14是一种新鉴定的TOG / XMAP215家族蛋白,与第二个同源物Dis1协同作用对于正确的染色体分离至关重要。我们表明,alp14突变体无法向正常的双极纺锤体形成。有趣的是,Alp14本身是Mad2依赖性纺锤体检查点级联的一个组成部分,因为添加微管去稳定剂后,alp14突变体无法维持高水平的H1激酶活性,从而导致安全蛋白破坏和染色体过早分离。 Alp14-绿色荧光蛋白的实时成像显示,在有丝分裂期间,Alp14与动植物的周围区域以及纺锤体极有关。 ChIP(染色质免疫沉淀)和与动粒标记Mis6重叠的定位支持了这一点。一个完整的纺锤体需要Alp14定位到线粒体外围,而不是两极。这些结果表明,TOG / XMAP215家族可能在动植物和极微管至染色体微管的正末端之间起桥梁的作用。

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