Endocytosis in malaria parasites: An ultrastructural perspective of membrane interplay in a unique infection model.

4区 生物学 Q4 Biochemistry, Genetics and Molecular Biology
Current topics in membranes Pub Date : 2024-01-01 Epub Date: 2024-08-05 DOI:10.1016/bs.ctm.2024.05.001
Camila Wendt, Kildare Miranda
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引用次数: 0

Abstract

Malaria remains a major global threat, representing a severe public health problem worldwide. Annually, it is responsible for a high rate of morbidity and mortality in many tropical developing countries where the disease is endemic. The causative agent of malaria, Plasmodium spp., exhibits a complex life cycle, alternating between an invertebrate vector, which transmits the disease, and the vertebrate host. The disease pathology observed in the vertebrate host is attributed to the asexual development of Plasmodium spp. inside the erythrocyte. Once inside the red blood cell, malaria parasites cause extensive changes in the host cell, increasing membrane rigidity and altering its normal discoid shape. Additionally, during their intraerythrocytic development, malaria parasites incorporate and degrade up to 70 % of host cell hemoglobin. This mechanism is essential for parasite development and represents an important drug target. Blocking the steps related to hemoglobin endocytosis or degradation impairs parasite development and can lead to its death. The ultrastructural analysis of hemoglobin endocytosis on Plasmodium spp. has been broadly explored along the years. However, it is only recently that the proteins involved in this process have started to emerge. Here, we will review the most important features related to hemoglobin endocytosis and catabolism on malaria parasites. A special focus will be given to the recent analysis obtained through 3D visualization approaches and to the molecules involved in these mechanisms.

疟原虫的内吞作用:从超微结构角度看独特感染模型中的膜相互作用
疟疾仍然是一个重大的全球性威胁,是全世界严重的公共卫生问题。在许多疟疾流行的热带发展中国家,疟疾每年都会造成很高的发病率和死亡率。疟疾的病原体疟原虫的生命周期十分复杂,在传播疾病的无脊椎病媒和脊椎动物宿主之间交替出现。在脊椎动物宿主身上观察到的疾病病理现象归因于疟原虫在红细胞内的无性发育。寄生在红细胞内的疟原虫会使宿主细胞发生巨大变化,增加细胞膜的硬度并改变其正常的盘状形状。此外,在红细胞内的发育过程中,疟原虫会吸收并降解宿主细胞中高达 70% 的血红蛋白。这一机制对寄生虫的发育至关重要,也是一个重要的药物靶点。阻断与血红蛋白内吞或降解有关的步骤会影响寄生虫的发育并导致其死亡。多年来,人们对疟原虫血红蛋白内吞的超微结构分析进行了广泛的探索。然而,参与这一过程的蛋白质直到最近才开始出现。在此,我们将回顾与疟原虫血红蛋白内吞和分解有关的最重要特征。我们将特别关注最近通过三维可视化方法获得的分析结果以及参与这些机制的分子。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Current topics in membranes
Current topics in membranes 生物-生化与分子生物学
CiteScore
3.50
自引率
0.00%
发文量
10
审稿时长
>12 weeks
期刊介绍: Current Topics in Membranes provides a systematic, comprehensive, and rigorous approach to specific topics relevant to the study of cellular membranes. Each volume is a guest edited compendium of membrane biology.
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