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牡蛎对疱疹病毒OsHV-1 μVar感染的代谢反应的蛋白质组学特征

Proteomic signatures of the oyster metabolic response to herpesvirus OsHV-1 μVar infection.

作者信息

Corporeau Charlotte, Tamayo David, Pernet Fabrice, Quéré Claudie, Madec Stéphanie

机构信息

Ifremer, Laboratoire des sciences de l'Environnement Marin (UMR 6539, LEMAR), 29280 Plouzané, France.

Ifremer, Laboratoire des sciences de l'Environnement Marin (UMR 6539, LEMAR), 29280 Plouzané, France; Departamento GAFFA (Animal Physiology), Facultad de Ciencia y Tecnología, Universidad del País Vasco/Euskal Herriko Unibertsitatea, Apartado 644, 48080 Bilbao, Spain.

出版信息

J Proteomics. 2014 Sep 23;109:176-87. doi: 10.1016/j.jprot.2014.06.030. Epub 2014 Jul 5.

Abstract

UNLABELLED

Pacific oyster Crassostrea gigas were inoculated with OsHV-1 at low load (control) or high load (challenged) to better understand the pathogenesis of ostreid herpesvirus 1 (OsHV-1 μVar) and to determine which metabolic pathways might be affected during infection. Animals were sampled for proteomic analysis two days post-injection, at the same time as OsHV-1 initiated an intense replication phase in challenged oysters. Twenty-five abundant protein spots that showed a marked change in accumulated levels were identified using a two-dimensional electrophoresis (2-DE) proteomic approach. Overall, these proteins are involved in cytoskeleton organization, protein turnover, induction of stress signals, signalling pathways and energy metabolism. Challenged oysters exhibited an increased glycolysis and VDAC accumulation, which reflect a "Warburg effect" as initially reported in cancer cells and more recently in shrimp infected with virus. The results presented here should be useful for identifying potential biomarkers of disease resistance and developing antiviral measures.

BIOLOGICAL SIGNIFICANCE

This study is the first 2-DE proteomic analysis dedicated to the pathogenesis of ostreid herpesvirus 1 (OsHV-1 μVar) in oyster Crassostrea gigas, the most important bivalve produced in the world. OsHV-1 has affected oysters every year since 2008. All the proteins identified in this paper are key targets involved in OsHV-1 infection processes. We presented evidence that the metabolic changes during infection in oyster somehow resemble the Warburg effect occurring in cancer cells. This work constitutes a real advance in the comprehension of the host metabolic pathways affected during OsHV-1 disease. Overall, this work contributes to a better understanding of disease mortalities in aquatic ecosystems which could guide management actions to mitigate their impacts.

摘要

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将太平洋牡蛎(Crassostrea gigas)以低负荷(对照)或高负荷(受挑战)接种1型牡蛎疱疹病毒(OsHV-1),以更好地了解牡蛎疱疹病毒1型(OsHV-1 μVar)的发病机制,并确定感染过程中哪些代谢途径可能受到影响。在注射后两天对动物进行采样以进行蛋白质组分析,此时OsHV-1在受挑战的牡蛎中开始进入强烈复制阶段。使用二维电泳(2-DE)蛋白质组学方法鉴定了25个积累水平有显著变化的丰富蛋白质斑点。总体而言,这些蛋白质参与细胞骨架组织、蛋白质周转、应激信号诱导、信号通路和能量代谢。受挑战的牡蛎表现出糖酵解增加和电压依赖性阴离子通道(VDAC)积累,这反映了最初在癌细胞中报道、最近在感染病毒的虾中发现的“瓦伯格效应”。此处呈现的结果应有助于识别抗病性的潜在生物标志物并制定抗病毒措施。

生物学意义

本研究是首次针对世界上最重要的双壳贝类——太平洋牡蛎(Crassostrea gigas)中牡蛎疱疹病毒1型(OsHV-1 μVar)发病机制的二维电泳蛋白质组分析。自2008年以来,OsHV-1每年都会感染牡蛎。本文鉴定的所有蛋白质都是参与OsHV-1感染过程的关键靶点。我们提供的证据表明,牡蛎感染期间的代谢变化在某种程度上类似于癌细胞中发生的瓦伯格效应。这项工作在理解OsHV-1疾病期间受影响的宿主代谢途径方面取得了实际进展。总体而言,这项工作有助于更好地理解水生生态系统中的疾病死亡率,从而指导管理行动以减轻其影响。

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