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Hotspots in Plasmodium and RBC Receptor-Ligand Interactions: Key Pieces for Inhibiting Malarial Parasite Invasion

机译:疟原虫和RBC受体-配体相互作用的热点:抑制疟原虫入侵的关键片断。

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摘要

Protein-protein interactions (IPP) play an essential role in practically all biological processes, including those related to microorganism invasion of their host cells. It has been found that a broad repertoire of receptor-ligand interactions takes place in the binding interphase with host cells in malaria, these being vital interactions for successful parasite invasion. Several trials have been conducted for elucidating the molecular interface of interactions between some and antigens with receptors on erythrocytes and/or reticulocytes. Structural information concerning these complexes is available; however, deeper analysis is required for correlating structural, functional (binding, invasion, and inhibition), and polymorphism data for elucidating new interaction hotspots to which malaria control methods can be directed. This review describes and discusses recent structural and functional details regarding three relevant interactions during erythrocyte invasion: Duffy-binding protein 1 (DBP1)–Duffy antigen receptor for chemokines (DARC); reticulocyte-binding protein homolog 5 ( Rh5)-basigin, and erythrocyte binding antigen 175 (EBA175)-glycophorin A (GPA).
机译:蛋白质-蛋白质相互作用(IPP)在几乎所有生物过程中都起着至关重要的作用,包括那些与微生物入侵其宿主细胞有关的过程。已经发现在疟疾中与宿主细胞的结合相中发生了广泛的受体-配体相互作用,这些是成功寄生虫入侵的重要相互作用。为了阐明一些抗原和抗原与红细胞和/或网状细胞上的受体之间的相互作用的分子界面,已经进行了一些试验。可获得有关这些配合物的结构信息;然而,需要更深入的分析来关联结构,功能(结合,侵袭和抑制)和多态性数据,以阐明可以控制疟疾方法的新的相互作用热点。这篇综述描述并讨论了有关红细胞入侵过程中三个相关相互作用的最新结构和功能细节:Duffy结合蛋白1(DBP1)–Duffy趋化因子抗原受体(DARC);网状细胞结合蛋白同源物5(Rh5)-basigin和红细胞结合抗原175(EBA175)-glycophorin A(GPA)。

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