The role of eIF2alpha phosphorylation in controlling intracellular development of Leishmania

eIF2α磷酸化在控制利什曼原虫细胞内发育中的作用

• 批准号: 418444-2012
• 负责人: Papadopoulou, Barbara
• 金额: $ 2.91万
• 依托单位: Université Laval
• 依托单位国家: 加拿大
• 项目类别: Discovery Grants Program - Individual
• 财政年份: 2016
• 资助国家: 加拿大
• 起止时间: 2016-01-01 至 2017-12-31
• 项目状态: 已结题
• 来源: https://www.nserc-crsng.gc.ca/ase-oro/Details-Detailles_eng.asp?id=596357
• 关键词: role; eIF2alpha; phosphorylation; controlling; intracellular

The parasitic protozoan Leishmania is the etiological agent of human leishmaniasis worldwide. Leishmania exists in two major developmental stages-free-living promastigotes in the sandfly vector and intracellular amastigotes in the phagolysosome of mammalian macrophages. During its differentiation from promastigote to amastigote forms, Leishmania experiences drastic environmental changes. In order for the parasite to differentiate and replicate within the harsh environment of the phagolysosome, it has to develop several adaptive responses/strategies involving important morphological and biochemical changes and dynamic alterations in the regulation of gene expression. In eukaryotes, one of the most conserved stress response pathways to control translation initiation is the phosphorylation of the alpha-subunit of eukaryotic initiation factor-2 by stress-responsive eIF2alpha kinases, resulting in the reduction of global translation. We have shown recently that eIF2alpha phosphorylation is a prerequisite for amastigote differentiation in macrophages. Slowly replicating amastigotes have to maintain translation rates low in order to adapt to stressful situations in the phagolysosome, such as acidic pH, nutritional and oxidative stresses. Decreased levels of translation in amastigotes coincide with eIF2alpha phosphorylation. Interestingly, we showed that phosphorylation of eIF2alpha is developmentally regulated by a novel cotranslational/ posttranslational mechanism. Such a regulation allows the insect promastigote form to proliferate faster but intracellular amastigotes to divide more slowly, as a strategy to adapt to a highly stressful and dynamic environment and to evade the immune response of the host macrophage. We propose a series of experiments to better understand the molecular mechanism(s) by which intracellular parasites respond to stress and ensure their survival. These studies will provide significant insights in the role that stress and eIF2alpha phosphorylation play in the development of intracellular pathogens.

利什曼原虫是世界范围内人类利什曼病的病原体。利什曼原虫存在于两个主要的发育阶段-白蛉载体中的自由生活的前鞭毛体和哺乳动物巨噬细胞吞噬溶酶体中的细胞内无鞭毛体。在利什曼原虫从前鞭毛体分化为无鞭毛体的过程中，它经历了剧烈的环境变化。为了使寄生虫在吞噬溶酶体的恶劣环境中分化和复制，它必须发展几种适应性反应/策略，包括重要的形态和生化变化以及基因表达调控的动态改变。在真核生物中，控制翻译起始的最保守的应激反应途径之一是应激反应性eIF 2 α激酶对真核生物起始因子-2的α亚基的磷酸化，导致整体翻译的减少。我们最近发现eIF 2 α磷酸化是巨噬细胞中无鞭毛体分化的先决条件。缓慢复制的无鞭毛体必须保持低的翻译速率，以适应吞噬溶酶体中的应激情况，例如酸性pH、营养和氧化应激。无鞭毛体中翻译水平的降低与eIF 2 α磷酸化一致。有趣的是，我们发现eIF 2 α的磷酸化是由一种新的共翻译/翻译后机制在发育过程中调节的。这种调节允许昆虫前鞭毛体形式更快地增殖，但细胞内无鞭毛体分裂更慢，作为适应高度应激和动态环境并逃避宿主巨噬细胞的免疫应答的策略。我们提出了一系列的实验，以更好地了解细胞内寄生虫响应压力，并确保其生存的分子机制。这些研究将为应激和eIF 2alpha磷酸化在细胞内病原体发展中的作用提供重要见解。