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一种新型基体蛋白是一种类Polo样激酶底物,对于布氏锥虫的基体分离和鞭毛附着是必需的。

A Novel Basal Body Protein That Is a Polo-like Kinase Substrate Is Required for Basal Body Segregation and Flagellum Adhesion in Trypanosoma brucei.

作者信息

Hu Huiqing, Zhou Qing, Li Ziyin

机构信息

From the Department of Microbiology and Molecular Genetics, University of Texas Medical School, Houston, Texas 77030.

From the Department of Microbiology and Molecular Genetics, University of Texas Medical School, Houston, Texas 77030

出版信息

J Biol Chem. 2015 Oct 9;290(41):25012-22. doi: 10.1074/jbc.M115.674796. Epub 2015 Aug 13.

Abstract

The Polo-like kinase (PLK) in Trypanosoma brucei plays multiple roles in basal body segregation, flagellum attachment, and cytokinesis. However, the mechanistic role of TbPLK remains elusive, mainly because most of its substrates are not known. Here, we report a new substrate of TbPLK, SPBB1, and its essential roles in T. brucei. SPBB1 was identified through yeast two-hybrid screening with the kinase-dead TbPLK as the bait. It interacts with TbPLK in vitro and in vivo, and is phosphorylated by TbPLK in vitro. SPBB1 localizes to both the mature basal body and the probasal body throughout the cell cycle, and co-localizes with TbPLK at the basal body during early cell cycle stages. RNAi against SPBB1 in procyclic trypanosomes inhibited basal body segregation, disrupted the new flagellum attachment zone filament, detached the new flagellum, and caused defective cytokinesis. Moreover, RNAi of SPBB1 confined TbPLK at the basal body and the bilobe structure, resulting in constitutive phosphorylation of TbCentrin2 at the bilobe. Altogether, these results identified a basal body protein as a TbPLK substrate and its essential role in promoting basal body segregation and flagellum attachment zone filament assembly for flagellum adhesion and cytokinesis initiation.

摘要

布氏锥虫中的类Polo样激酶(PLK)在基体分离、鞭毛附着和胞质分裂中发挥多种作用。然而,TbPLK的作用机制仍不清楚,主要是因为其大多数底物尚不清楚。在此,我们报道了TbPLK的一种新底物SPBB1及其在布氏锥虫中的重要作用。通过以激酶失活的TbPLK为诱饵进行酵母双杂交筛选鉴定出SPBB1。它在体外和体内均与TbPLK相互作用,并在体外被TbPLK磷酸化。在整个细胞周期中,SPBB1定位于成熟基体和原基体,在细胞周期早期阶段与TbPLK在基体处共定位。对前循环型锥虫中SPBB1进行RNA干扰会抑制基体分离,破坏新的鞭毛附着区丝,使新鞭毛脱离,并导致胞质分裂缺陷。此外,SPBB1的RNA干扰将TbPLK限制在基体和双叶结构处,导致双叶处的TbCentrin2发生组成型磷酸化。总之,这些结果确定了一种基体蛋白作为TbPLK的底物,及其在促进基体分离和鞭毛附着区丝组装以实现鞭毛黏附和胞质分裂起始中的重要作用。

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