Department of Microbiology and Molecular Genetics, McGovern Medical School, University of Texas Health Science Center at Houston, Houston, TX, United States of America.
PLoS Pathog. 2018 May 29;14(5):e1007101. doi: 10.1371/journal.ppat.1007101. eCollection 2018 May.
Trypanosoma brucei undergoes life cycle form transitions from trypomastigotes to epimastigotes in the insect vector by re-positioning the mitochondrial genome and re-locating the flagellum and flagellum-associated cytoskeletal structures. The mechanism underlying these dramatic morphology transitions remains poorly understood. Here we report the regulatory role of the orphan kinesin KIN-E in controlling trypanosome morphology transitions. KIN-E localizes to the flagellum and is enriched at the flagellar tip, and this localization depends on the C-terminal m-calpain domain III-like domains. Depletion of KIN-E in the trypomastigote form of T. brucei causes major morphology changes and a gradual increase in the level of EP procyclin, generating epimastigote-like cells. Mechanistically, through its C-terminal importin α-like domain, KIN-E targets FLAM3, a flagellar protein involved in morphology transitions, to the flagellum to promote elongation of the flagellum attachment zone and positioning of the flagellum and flagellum-associated cytoskeletal structure, thereby maintaining trypomastigote cell morphology. Our findings suggest that morphology transitions in trypanosomes require KIN-E-mediated transport of FLAM3 to the flagellum.
布氏锥虫通过重新定位线粒体基因组和重新定位鞭毛和鞭毛相关细胞骨架结构,从锥虫体向锥鞭毛体进行生命周期形态转变。这些戏剧性的形态转变的机制仍知之甚少。在这里,我们报告了孤儿驱动蛋白 KIN-E 在控制锥虫形态转变中的调节作用。KIN-E 定位于鞭毛上,并在鞭毛尖端富集,这种定位依赖于 C 末端 m-calpain 结构域 III 样结构域。在布氏锥虫的锥虫体形式中耗尽 KIN-E 会导致主要的形态变化和 EP 前鞭毛蛋白水平的逐渐增加,从而产生锥鞭毛体样细胞。在机制上,通过其 C 末端输入蛋白α样结构域,KIN-E 将参与形态转变的鞭毛蛋白 FLAM3 靶向到鞭毛上,以促进鞭毛附着区的伸长和鞭毛及鞭毛相关细胞骨架结构的定位,从而维持锥虫体的形态。我们的发现表明,锥虫的形态转变需要 KIN-E 介导的 FLAM3 向鞭毛的运输。
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