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PP2A-Twins Is Antagonized by Greatwall and Collaborates with Polo for Cell Cycle Progression and Centrosome Attachment to Nuclei in Drosophila Embryos

机译:PP2A-双胞胎被长城(Greatwall)拮抗,并与马球菌(Polo)合作进行果蝇胚胎细胞周期进程和中心体附着于细胞核的过程。

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Cell division and development are regulated by networks of kinases and phosphatases. In early Drosophila embryogenesis, 13 rapid nuclear divisions take place in a syncytium, requiring fine coordination between cell cycle regulators. The Polo kinase is a conserved, crucial regulator of M-phase. We have recently reported an antagonism between Polo and Greatwall (Gwl), another mitotic kinase, in Drosophila embryos. However, the nature of the pathways linking them remained elusive. We have conducted a comprehensive screen for additional genes functioning with polo and gwl. We uncovered a strong interdependence between Polo and Protein Phosphatase 2A (PP2A) with its B-type subunit Twins (Tws). Reducing the maternal contribution of Polo and PP2A-Tws together is embryonic lethal. We found that Polo and PP2A-Tws collaborate to ensure centrosome attachment to nuclei. While a reduction in Polo activity leads to centrosome detachments observable mostly around prophase, a reduction in PP2A-Tws activity leads to centrosome detachments at mitotic exit, and a reduction in both Polo and PP2A-Tws enhances the frequency of detachments at all stages. Moreover, we show that Gwl antagonizes PP2A-Tws function in both meiosis and mitosis. Our study highlights how proper coordination of mitotic entry and exit is required during embryonic cell cycles and defines important roles for Polo and the Gwl-PP2A-Tws pathway in this process.
机译:细胞分裂和发育受激酶和磷酸酶网络调节。在果蝇早期胚胎发生中,合胞体发生13个快速核分裂,需要细胞周期调节剂之间的良好协调。 Polo激酶是M期的保守,关键调节剂。我们最近报道了果蝇胚胎中Polo和另一种有丝分裂激酶长城(Gwl)之间的拮抗作用。但是,连接它们的途径的性质仍然难以捉摸。我们已经对带有polo和gwl的其他基因进行了全面的筛选。我们发现Polo和蛋白磷酸酶2A(PP2A)及其B型亚基Twins(Tws)之间存在强烈的相互依赖性。一起降低Polo和PP2A-Tws的母亲贡献是胚胎致死的。我们发现Polo和PP2A-Tws协作以确保中心体附着在核上。虽然Polo活性的降低导致大部分在前期可观察到的中心体脱离,但PP2A-Tws活性的降低导致有丝分裂出口处的中心体脱离,而Polo和PP2A-Tws的降低都增加了各个阶段的脱离频率。此外,我们表明,Gwl拮抗PP2A-Tws在减数分裂和有丝分裂中的功能。我们的研究突出了在胚胎细胞周期中需要如何正确协调有丝分裂的进入和退出,并定义了Polo和Gwl-PP2A-Tws途径在此过程中的重要作用。

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