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疟原虫 PfEMP1 外排途径的时空映射。

Spatial and temporal mapping of the PfEMP1 export pathway in Plasmodium falciparum.

机构信息

Department of Biochemistry and Molecular Biology, The University of Melbourne, Melbourne, Victoria, Australia.

出版信息

Cell Microbiol. 2013 Aug;15(8):1401-18. doi: 10.1111/cmi.12125. Epub 2013 Mar 14.

Abstract

The human malaria parasite, Plasmodium falciparum, modifies the red blood cells (RBCs) that it infects by exporting proteins to the host cell. One key virulence protein, P. falciparum Erythrocyte Membrane Protein-1 (PfEMP1), is trafficked to the surface of the infected RBC, where it mediates adhesion to the vascular endothelium. We have investigated the organization and development of the exomembrane system that is used for PfEMP1 trafficking. Maurer's cleft cisternae are formed early after invasion and proteins are delivered to these (initially mobile) structures in a temporally staggered and spatially segregated manner. Membrane-Associated Histidine-Rich Protein-2 (MAHRP2)-containing tether-like structures are generated as early as 4 h post invasion and become attached to Maurer's clefts. The tether/Maurer's cleft complex docks onto the RBC membrane at ~20 h post invasion via a process that is not affected by cytochalasin D treatment. We have examined the trafficking of a GFP chimera of PfEMP1 expressed in transfected parasites. PfEMP1B-GFP accumulates near the parasite surface, within membranous structures exhibiting a defined ultrastructure, before being transferred to pre-formed mobile Maurer's clefts. Endogenous PfEMP1 and PfEMP1B-GFP are associated with Electron-Dense Vesicles that may be responsible for trafficking PfEMP1 from the Maurer's clefts to the RBC membrane.

摘要

人类疟疾寄生虫疟原虫通过向宿主细胞输出蛋白来修饰它感染的红细胞(RBC)。一种关键的毒力蛋白,疟原虫红细胞膜蛋白 1(PfEMP1),被运输到受感染的 RBC 的表面,在那里它介导与血管内皮的粘附。我们研究了用于 PfEMP1 运输的外膜系统的组织和发育。入侵后早期形成 Maurer 裂隙潴泡,蛋白质以时间交错和空间分隔的方式递送到这些(最初是可移动的)结构中。膜相关组氨酸丰富蛋白 2(MAHRP2)包含的系绳样结构早在入侵后 4 小时就产生,并附着在 Maurer 裂隙上。系绳/Maurer 裂隙复合物通过一个不受细胞松弛素 D 处理影响的过程,在入侵后约 20 小时与 RBC 膜对接。我们检查了在转染寄生虫中表达的 GFP 嵌合 PfEMP1 的运输。PfEMP1B-GFP 在被转移到预先形成的可移动 Maurer 裂隙之前,在寄生虫表面附近积累,在膜状结构中表现出明确的超微结构。内源性 PfEMP1 和 PfEMP1B-GFP 与电子致密小泡相关,这些小泡可能负责将 PfEMP1 从 Maurer 裂隙转运到 RBC 膜。

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