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非洲锥虫中恒定表面跨膜结构域蛋白循环利用的证据。

Evidence for recycling of invariant surface transmembrane domain proteins in African trypanosomes.

作者信息

Koumandou V Lila, Boehm Cordula, Horder Katy A, Field Mark C

机构信息

Department of Pathology, University of Cambridge, Cambridge, United Kingdom.

出版信息

Eukaryot Cell. 2013 Feb;12(2):330-42. doi: 10.1128/EC.00273-12. Epub 2012 Dec 21.

Abstract

Intracellular trafficking is a vital component of both virulence mechanisms and drug interactions in Trypanosoma brucei, the causative agent of human African trypanosomiasis and n'agana of cattle. Both maintaining the surface proteome composition within a life stage and remodeling the composition when progressing between life stages are important features of immune evasion and development for trypanosomes. Our recent work implicates the abundant transmembrane invariant surface glycoproteins (ISGs) in the uptake of first-line therapeutic suramin, suggesting a potential therapeutic route into the cell. RME-8 is a mediator of recycling pathways in higher eukaryotes and is one of a small cohort of intracellular transport gene products upregulated in mammal-infective trypanosomes, suggesting a role in controlling the copy number of surface proteins in trypanosomes. Here we investigate RME-8 function and its contribution to intracellular trafficking and stability of ISGs. RME-8 is a highly conserved protein and is broadly distributed across multiple endocytic compartments. By knockdown we find that RME-8 is essential and mediates delivery of endocytic probes to late endosomal compartments. Further, we find ISG accumulation within endosomes, but that RME-8 knockdown also increases ISG turnover; combined with previous data, this suggests that it is most probable that ISGs are recycled, and that RME-8 is required to support recycling.

摘要

细胞内运输是布氏锥虫(人类非洲锥虫病和牛那加那病的病原体)毒力机制和药物相互作用的重要组成部分。在一个生命阶段维持表面蛋白质组组成以及在不同生命阶段转换时重塑组成,都是锥虫逃避免疫和发育的重要特征。我们最近的研究表明,丰富的跨膜不变表面糖蛋白(ISG)参与了一线治疗药物苏拉明的摄取,这提示了一条潜在的进入细胞的治疗途径。RME-8是高等真核生物中回收途径的介导因子,是在感染哺乳动物的锥虫中上调的一小群细胞内运输基因产物之一,这表明它在控制锥虫表面蛋白拷贝数方面发挥作用。在这里,我们研究RME-8的功能及其对细胞内运输和ISG稳定性的贡献。RME-8是一种高度保守的蛋白质,广泛分布于多个内吞区室。通过敲低实验,我们发现RME-8是必需的,并且介导内吞探针向晚期内体区室的递送。此外,我们发现内体中有ISG积累,但RME-8敲低也会增加ISG的周转;结合先前的数据,这表明ISG最有可能被回收,并且RME-8是支持回收所必需的。

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