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A Functional Analysis of the Cyclophilin Repertoire in the Protozoan Parasite Trypanosoma Cruzi

机译:原生动物寄生虫克氏锥虫亲环蛋白库的功能分析

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摘要

Trypanosoma cruzi is the etiological agent of Chagas disease. It affects eight million people worldwide and can be spread by several routes, such as vectorborne transmission in endemic areas and congenitally, and is also important in non-endemic regions such as the United States and Europe due to migration from Latin America. Cyclophilins (CyPs) are proteins with enzymatic peptidyl-prolyl isomerase activity (PPIase), essential for protein folding in vivo. Cyclosporin A (CsA) has a high binding affinity for CyPs and inhibits their PPIase activity. CsA has proved to be a parasiticidal drug on some protozoa, including T. cruzi. In this review, we describe the T. cruzi cyclophilin gene family, that comprises 15 paralogues. Among the proteins isolated by CsA-affinity chromatography, we found orthologues of mammalian CyPs. TcCyP19, as the human CyPA, is secreted to the extracellular environment by all parasite stages and could be part of a complex interplay involving the parasite and the host cell. TcCyP22, an orthologue of mitochondrial CyPD, is involved in the regulation of parasite cell death. Our findings on T. cruzi cyclophilins will allow further characterization of these processes, leading to new insights into the biology, the evolution of metabolic pathways, and novel targets for anti-T. cruzi control.
机译:克氏锥虫是南美锥虫病的病原体。它影响着全球八百万人,可以通过多种途径传播,例如在流行地区和先天性传播媒介传播,由于从拉丁美洲的迁移,它在非流行地区(例如美国和欧洲)也很重要。亲环蛋白(CyPs)是具有酶促肽基脯氨酰异构酶活性(PPIase)的蛋白,对于体内蛋白折叠至关重要。环孢菌素A(CsA)对CyP具有高结合亲和力,并抑制其PPIase活性。 CsA已被证明是对某些原生动物(包括克鲁氏锥虫)的杀虫药。在这篇综述中,我们描述了包括15个旁系同源物的克氏锥虫亲环蛋白基因家族。在通过CsA亲和层析分离的蛋白质中,我们发现了哺乳动物CyP的直向同源物。 TcCyP19,作为人类CyPA,在所有寄生虫阶段都分泌到细胞外环境中,并且可能是涉及寄生虫和宿主细胞的复杂相互作用的一部分。 TcCyP22,线粒体CyPD的直系同源物,参与寄生虫细胞死亡的调控。我们对克鲁斯氏锥虫亲环蛋白的发现将允许对这些过程进行进一步的表征,从而获得对生物学的新见解,新陈代谢途径的发展以及抗T的新靶标。克鲁兹控制。

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