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Host Erythrocyte Environment Influences the Localization of Exported Protein 2 an Essential Component of the Plasmodium Translocon

机译:宿主红细胞环境影响出口蛋白2疟原虫Translocon的基本组成部分的本地化。

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摘要

Malaria parasites replicating inside red blood cells (RBCs) export a large subset of proteins into the erythrocyte cytoplasm to facilitate parasite growth and survival. PTEX, the parasite-encoded translocon, mediates protein transport across the parasitophorous vacuolar membrane (PVM) in Plasmodium falciparum-infected erythrocytes. Proteins exported into the erythrocyte cytoplasm have been localized to membranous structures, such as Maurer's clefts, small vesicles, and a tubovesicular network. Comparable studies of protein trafficking in Plasmodium vivax-infected reticulocytes are limited. With Plasmodium yoelii-infected reticulocytes, we identified exported protein 2 (Exp2) in a proteomic screen of proteins putatively transported across the PVM. Immunofluorescence studies showed that P. yoelii Exp2 (PyExp2) was primarily localized to the PVM. Unexpectedly, PyExp2 was also associated with distinct, membrane-bound vesicles in the reticulocyte cytoplasm. This is in contrast to P. falciparum in mature RBCs, where P. falciparum Exp2 (PfExp2) is exclusively localized to the PVM. Two P. yoelii-exported proteins, PY04481 (encoded by a pyst-a gene) and PY06203 (PypAg-1), partially colocalized with these PyExp2-positive vesicles. Further analysis revealed that with P. yoelii, Plasmodium berghei, and P. falciparum, cytoplasmic Exp2-positive vesicles were primarily observed in CD71+ reticulocytes versus mature RBCs. In transgenic P. yoelii 17X parasites, the association of hemagglutinin-tagged PyExp2 with the PVM and cytoplasmic vesicles was retained, but the pyexp2 gene was refractory to deletion. These data suggest that the localization of Exp2 in mouse and human RBCs can be influenced by the host cell environment. Exp2 may function at multiple points in the pathway by which parasites traffic proteins into and through the reticulocyte cytoplasm.
机译:在红细胞(RBC)中复制的疟原虫将大量蛋白质输出到红细胞胞质中,以促进寄生虫的生长和存活。 PTEX是寄生虫编码的转位子,可在恶性疟原虫感染的红细胞中介导穿过寄生虫液泡膜(PVM)的蛋白质运输。出口到红细胞胞质中的蛋白质已定位于膜结构,例如毛勒氏裂,小囊泡和肾小管网络。在间日疟原虫感染的网织红细胞中蛋白质运输的可比研究是有限的。用约氏疟原虫感染的网织红细胞,我们在蛋白质组学筛选中推定跨过PVM转运的蛋白质中鉴定了输出蛋白质2(Exp2)。免疫荧光研究表明,约氏疟原虫Exp2(PyExp2)主要位于PVM。出乎意料的是,PyExp2还与网织红细胞细胞质中独特的,膜结合的囊泡相关。这与成熟RBC中的恶性疟原虫相反,恶性疟原虫Exp2(PfExp2)仅局限在PVM中。两个约氏疟原虫输出蛋白PY04481(由pyst-a基因编码)和PY06203(PypAg-1)与这些PyExp2阳性囊泡部分共定位。进一步的分析表明,与成熟的红细胞相比,约氏疟原虫,柏氏疟原虫和恶性疟原虫主要在CD71 + 网织细胞中观察到胞质的Exp2阳性囊泡。在转基因 P。 yoelii 17X寄生虫保留了血凝素标记的 Py Exp2与PVM和细胞质囊泡的关联,但 pyexp2 基因难以删除。这些数据表明,Exp2在小鼠和人类RBC中的定位会受到宿主细胞环境的影响。 Exp2可能在途径中的多个点起作用,寄生虫通过这些途径将蛋白质运输到网状细胞质中并通过网状细胞质。

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