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Proteomic profiling of the outer membrane fraction of the obligate intracellular bacterial pathogen ehrlichia ruminantium

机译:专性细胞内细菌病原体反刍动物反刍动物外膜部分的蛋白质组学分析

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摘要

The outer membrane proteins (OMPs) of Gram-negative bacteria play a crucial role in virulence and pathogenesis. Identification of these proteins represents an important goal for bacterial proteomics, because it aids in vaccine development. Here, we have developed such an approach for Ehrlichia ruminantium, the obligate intracellular bacterium that causes heartwater. A preliminary whole proteome analysis of elementary bodies, the extracellular infectious form of the bacterium, had been performed previously, but information is limited about OMPs in this organism and about their role in the protective immune response. Identification of OMPs is also essential for understanding Ehrlichia's OM architecture, and how the bacterium interacts with the host cell environment. First, we developed an OMP extraction method using the ionic detergent sarkosyl, which enriched the OM fraction. Second, proteins were separated via one-dimensional electrophoresis, and digested peptides were analyzed via nano-liquid chromatographic separation coupled with mass spectrometry (LC-MALDI-TOF/TOF). Of 46 unique proteins identified in the OM fraction, 18 (39%) were OMPs, including 8 proteins involved in cell structure and biogenesis, 4 in transport/virulence, 1 porin, and 5 proteins of unknown function. These experimental data were compared to the predicted subcellular localization of the entire E. ruminantium proteome, using three different algorithms. This work represents the most complete proteome characterization of the OM fraction in Ehrlichia spp. The study indicates that suitable subcellular fractionation experiments combined with straightforward computational analysis approaches are powerful for determining the predominant subcellular localization of the experimentally observed proteins. We identified proteins potentially involved in E. ruminantium pathogenesis, which are good novel targets for candidate vaccines. Thus, combining bioinformatics and investigating new vaccines against this organism. In summary, we provide both pioneering data and novel insights into the pathogenesis of this obligate intracellular bacterium.
机译:革兰氏阴性细菌的外膜蛋白(OMP)在毒力和发病机理中起着至关重要的作用。这些蛋白质的鉴定代表了细菌蛋白质组学的重要目标,因为它有助于疫苗的开发。在这里,我们已经开发了一种用于反刍毛虫埃希氏毛虫的方法,这是引起心水的专性细胞内细菌。先前已经对细菌的细胞外感染形式即基本体进行了初步的整体蛋白质组分析,但是有关该生物体中OMP及其在保护性免疫应答中的作用的信息有限。 OMP的鉴定对于理解埃希氏菌属的OM结构以及细菌如何与宿主细胞环境相互作用也至关重要。首先,我们开发了使用离子型洗涤剂Sarkosyl提取OMP的方法,该方法丰富了OM馏分。其次,通过一维电泳分离蛋白质,并通过纳米液相色谱分离和质谱联用(LC-MALDI-TOF / TOF)分析消化的肽。在OM组分中鉴定出的46种独特蛋白中,有18种(占39%)是OMP,包括8种参与细胞结构和生物发生的蛋白,4种转运/毒力蛋白,1种孔蛋白和5种功能未知的蛋白。使用三种不同的算法,将这些实验数据与预测的整个反刍动物蛋白质组的亚细胞定位进行了比较。这项工作代表了埃里希氏菌属OM组分最完整的蛋白质组学表征。该研究表明,合适的亚细胞分级分离实验与直接的计算分析方法相结合,对于确定实验观察到的蛋白质的主要亚细胞定位非常有力。我们确定了潜在的与大肠埃希菌的发病机理有关的蛋白质,它们是候选疫苗的良好新靶标。因此,结合生物信息学并研究针对这种生物的新疫苗。总而言之,我们提供了开创性的数据和这种专性细胞内细菌发病机理的新颖见解。

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