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光滑双脐螺的两种寄生虫——曼氏血吸虫幼虫和卡氏棘口吸虫的排泄分泌蛋白质组

Excretory-secretory proteome of larval Schistosoma mansoni and Echinostoma caproni, two parasites of Biomphalaria glabrata.

作者信息

Guillou François, Roger Emmanuel, Moné Yves, Rognon Anne, Grunau Christoph, Théron André, Mitta Guillaume, Coustau Christine, Gourbal Benjamin E F

机构信息

Parasitologie Fonctionnelle et Evolutive, UMR 5244, CNRS Université de Perpignan, 52 Ave Paul Alduy, 66860 Perpignan Cedex, France.

出版信息

Mol Biochem Parasitol. 2007 Sep;155(1):45-56. doi: 10.1016/j.molbiopara.2007.05.009. Epub 2007 May 29.

DOI:10.1016/j.molbiopara.2007.05.009
PMID:17606306
Abstract

Schistosoma mansoni and Echinostoma caproni are two trematode species that use different strategies (mimicry and immunosuppression, respectively) to interfere with the snail innate immune system. Parasites excretory-secretory (ES) products have been shown to play a key role in these host-parasite immune interactions. However, they remain largely uncharacterized in larval trematodes. We developed a global proteomic approach to characterize the ES proteome of S. mansoni and E. caproni primary sporocysts. In ES products of both parasites, we found proteins involved in reactive oxygen species scavenging, glycolysis, signalling or calcium binding (superoxide dismutase Cu/Zn; glutathione S-transferase; aldo-keto-reductase; triose-phosphate isomerase; glyceraldehyde-3-phosphate dehydrogenase; aldolase, enolase, MICAL-like, calreticulin). According to their predicted functions, we propose a model in which these proteins (i) are involved in antioxidant activity, (ii) prevent hemocyte encapsulation process or (iii) favor invasion and migration of sporocysts in host tissues. These results suggest that S. mansoni and E. caproni sporocysts develope a strong immune protection during the first hours of infection giving them enough time to build up a long lasting immune evasion strategy relying on molecular mimicry or immunosuppression, respectively.

摘要

曼氏血吸虫和卡氏棘口吸虫是两种吸虫,它们分别采用不同策略(模仿和免疫抑制)来干扰蜗牛的先天免疫系统。寄生虫的排泄-分泌(ES)产物已被证明在这些宿主-寄生虫免疫相互作用中起关键作用。然而,在幼虫吸虫中它们在很大程度上仍未得到充分表征。我们开发了一种全局蛋白质组学方法来表征曼氏血吸虫和卡氏棘口吸虫初级孢蚴的ES蛋白质组。在这两种寄生虫的ES产物中,我们发现了参与活性氧清除、糖酵解、信号传导或钙结合的蛋白质(铜/锌超氧化物歧化酶;谷胱甘肽S-转移酶;醛糖酮还原酶;磷酸丙糖异构酶;甘油醛-3-磷酸脱氢酶;醛缩酶、烯醇化酶、类MICAL蛋白、钙网蛋白)。根据它们的预测功能,我们提出了一个模型,其中这些蛋白质(i)参与抗氧化活性,(ii)阻止血细胞包囊过程,或(iii)促进孢蚴在宿主组织中的侵入和迁移。这些结果表明,曼氏血吸虫和卡氏棘口吸虫孢蚴在感染的最初几个小时内形成了强大的免疫保护,使它们有足够的时间分别依靠分子模仿或免疫抑制建立长期的免疫逃避策略。

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