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Survey of Surface Proteins from the Pathogenic Mycoplasma hyopneumoniae Strain 7448 Using a Biotin Cell Surface Labeling Approach

机译:使用生物素细胞表面标记方法调查致病性猪肺炎支原体菌株7448的表面蛋白

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摘要

The characterization of the repertoire of proteins exposed on the cell surface by Mycoplasma hyopneumoniae (M. hyopneumoniae), the etiological agent of enzootic pneumonia in pigs, is critical to understand physiological processes associated with bacterial infection capacity, survival and pathogenesis. Previous in silico studies predicted that about a third of the genes in the M. hyopneumoniae genome code for surface proteins, but so far, just a few of them have experimental confirmation of their expression and surface localization. In this work, M. hyopneumoniae surface proteins were labeled in intact cells with biotin, and affinity-captured biotin-labeled proteins were identified by a gel-based liquid chromatography-tandem mass spectrometry approach. A total of 20 gel slices were separately analyzed by mass spectrometry, resulting in 165 protein identifications corresponding to 59 different protein species. The identified surface exposed proteins better defined the set of M. hyopneumoniae proteins exposed to the host and added confidence to in silico predictions. Several proteins potentially related to pathogenesis, were identified, including known adhesins and also hypothetical proteins with adhesin-like topologies, consisting of a transmembrane helix and a large tail exposed at the cell surface. The results provided a better picture of the M. hyopneumoniae cell surface that will help in the understanding of processes important for bacterial pathogenesis. Considering the experimental demonstration of surface exposure, adhesion-like topology predictions and absence of orthologs in the closely related, non-pathogenic species Mycoplasma flocculare, several proteins could be proposed as potential targets for the development of drugs, vaccines and/or immunodiagnostic tests for enzootic pneumonia.
机译:猪肺炎支原体肺炎的病原体猪支原体肺炎支原体(M. hyopneumoniae)暴露在细胞表面的蛋白质种类的表征对于理解与细菌感染能力,存活和发病机理相关的生理过程至关重要。先前的计算机模拟研究预测,猪肺炎支原体基因组中约有三分之一的基因编码表面蛋白,但到目前为止,只有其中的少数几个在实验上证实了它们的表达和表面定位。在这项工作中,猪肺炎支原体表面蛋白在完整细胞中用生物素标记,并通过基于凝胶的液相色谱-串联质谱法鉴定了亲和力捕获的生物素标记蛋白。通过质谱法分别对总共20个凝胶切片进行了分析,得到165种蛋白质鉴定,分别对应59种不同的蛋白质。鉴定出的表面暴露蛋白更好地定义了暴露于宿主的猪肺炎支原体蛋白的集合,并增加了计算机预测的信心。鉴定了几种可能与发病机制有关的蛋白质,包括已知的粘附素,以及具有粘附素样拓扑结构的假想蛋白质,其由跨膜螺旋和暴露于细胞表面的大尾巴组成。结果为猪肺炎支原体细胞表面提供了更好的图像,这将有助于理解对细菌发病机理重要的过程。考虑到表面暴露,类似粘附的拓扑结构预测的实验证明以及在紧密相关的非致病性物种Mycoplasma flocculare中直系同源物的缺失,可以提出几种蛋白质作为开发药物,疫苗和/或免疫诊断测试的潜在靶标地方性肺炎。

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