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Essential Roles for GPI-anchored Proteins in African Trypanosomes Revealed Using Mutants Deficient in GPI8

机译:GPI锚定的蛋白质在非洲锥虫中的重要作用,使用缺乏GPI8的突变体来揭示。

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摘要

The survival of Trypanosoma brucei, the causative agent of Sleeping Sickness and Nagana, is facilitated by the expression of a dense surface coat of glycosylphosphatidylinositol (GPI)-anchored proteins in both its mammalian and tsetse fly hosts. We have characterized T. brucei GPI8, the gene encoding the catalytic subunit of the GPI:protein transamidase complex that adds preformed GPI anchors onto nascent polypeptides. Deletion of GPI8 (to give Δgpi8) resulted in the absence of GPI-anchored proteins from the cell surface of procyclic form trypanosomes and accumulation of a pool of non–protein-linked GPI molecules, some of which are surface located. Procyclic Δgpi8, while viable in culture, were unable to establish infections in the tsetse midgut, confirming that GPI-anchored proteins are essential for insect-parasite interactions. Applying specific inducible GPI8 RNAi with bloodstream form parasites resulted in accumulation of unanchored variant surface glycoprotein and cell death with a defined multinuclear, multikinetoplast, and multiflagellar phenotype indicative of a block in cytokinesis. These data show that GPI-anchored proteins are essential for the viability of bloodstream form trypanosomes even in the absence of immune challenge and imply that GPI8 is important for proper cell cycle progression.
机译:昏睡病和长假病的病原体布鲁氏锥虫的生存,是通过在其哺乳动物和采采蝇蝇寄主中糖基磷脂酰肌醇(GPI)锚定蛋白的致密表层表达而促进的。我们已经表征了布鲁氏杆菌GPI8,该基因编码GPI:蛋白质转酰胺酶复合物的催化亚基,该复合物将预先形成的GPI锚添加到新生多肽上。 GPI8的缺失(给出Δgpi8)导致前环形式锥虫体细胞表面不存在GPI锚定蛋白,并且堆积了一些非蛋白连接的GPI分子,其中一些位于表面。前环Δgpi8虽然在培养中可行,但无法在采采蝇中肠建立感染,这证明GPI锚定的蛋白质对于昆虫与寄生虫的相互作用至关重要。将特定的可诱导GPI8 RNAi与血流形式的寄生虫一起使用会导致未锚定变体表面糖蛋白的积累和细胞死亡,并伴有明确的多核,多动素体和多鞭毛表型,表明胞质分裂受阻。这些数据表明,即使在没有免疫攻击的情况下,GPI锚定的蛋白对于血流形式锥虫的生存力也是必不可少的,这暗示GPI8对于适当的细胞周期进程很重要。

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