首页> 美国卫生研究院文献>The Journal of Biophysical and Biochemical Cytology >HURP permits MTOC sorting for robust meiotic spindle bipolarity similar to extra centrosome clustering in cancer cells
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HURP permits MTOC sorting for robust meiotic spindle bipolarity similar to extra centrosome clustering in cancer cells

机译:HURP允许MTOC分选以实现稳健的减数分裂纺锤体双极性类似于癌细胞中的额外中心体簇

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摘要

In contrast to somatic cells, formation of acentriolar meiotic spindles relies on the organization of microtubules (MTs) and MT-organizing centers (MTOCs) into a stable bipolar structure. The underlying mechanisms are still unknown. We show that this process is impaired in hepatoma up-regulated protein (Hurp) knockout mice, which are viable but female sterile, showing defective oocyte divisions. HURP accumulates on interpolar MTs in the vicinity of chromosomes via Kinesin-5 activity. By promoting MT stability in the spindle central domain, HURP allows efficient MTOC sorting into distinct poles, providing bipolarity establishment and maintenance. Our results support a new model for meiotic spindle assembly in which HURP ensures assembly of a central MT array, which serves as a scaffold for the genesis of a robust bipolar structure supporting efficient chromosome congression. Furthermore, HURP is also required for the clustering of extra centrosomes before division, arguing for a shared molecular requirement of MTOC sorting in mammalian meiosis and cancer cell division.
机译:与体细胞相反,人绒毛膜减数分裂纺锤体的形成依赖于微管(MTs)和MT组织中心(MTOCs)组织成稳定的双极结构。潜在的机制仍然未知。我们显示此过程在肝癌上调蛋白(Hurp)敲除小鼠中受损,这些小鼠是可行的但雌性不育,表现出有缺陷的卵母细胞分裂。 HURP通过Kinesin-5活性积聚在染色体附近的极间MTs上。通过提高主轴中心域的MT稳定性,HURP可以将MTOC有效地分类到不同的极点,从而建立和维护双极性。我们的研究结果支持减数分裂纺锤体组装的新模型,其中HURP确保组装中央MT阵列,该阵列可作为支持高效染色体国会的强大双极结构发生的支架。此外,HURP还需要在分裂之前将多余的中心体聚集在一起,这是哺乳动物减数分裂和癌细胞分裂中MTOC分选的共同分子要求。

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