首页> 外文期刊>Clinical and vaccine immunology: CVI >Characterization of anti-Salmonella enterica serotype Typhi antibody responses in bacteremic Bangladeshi patients by an immunoaffinity proteomics-based technology.
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Characterization of anti-Salmonella enterica serotype Typhi antibody responses in bacteremic Bangladeshi patients by an immunoaffinity proteomics-based technology.

机译:特性列阵的血清在bacteremic伤寒血清型抗体反应由immunoaffinity孟加拉国的病人proteomics-based技术。

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Salmonella enterica serotype Typhi is the cause of typhoid fever and a human-restricted pathogen. Currently available typhoid vaccines provide 50 to 90% protection for 2 to 5 years, and available practical diagnostic assays to identify individuals with typhoid fever lack sensitivity and/or specificity. Identifying immunogenic S. Typhi antigens expressed during human infection could lead to improved diagnostic assays and vaccines. Here we describe a platform immunoaffinity proteomics-based technology (IPT) that involves the use of columns charged with IgG, IgM, or IgA antibody fractions recovered from humans bacteremic with S. Typhi to capture S. Typhi proteins that were subsequently identified by mass spectrometry. This screening tool identifies immunogenic proteins recognized by antibodies from infected hosts. Using this technology and the plasma of patients with S. Typhi bacteremia in Bangladesh, we identified 57 proteins of S. Typhi, including proteins known to be immunogenic (PagC, HlyE, OmpA, and GroEL) and a number of proteins present in the human-restricted serotypes S. Typhi and S. Paratyphi A but rarely found in broader-host-range Salmonella spp. (HlyE, CdtB, PltA, and STY1364). We categorized identified proteins into a number of major groupings, including those involved in energy metabolism, protein synthesis, iron homeostasis, and biosynthetic and metabolic functions and those predicted to localize to the outer membrane. We assessed systemic and mucosal anti-HlyE responses in S. Typhi-infected patients and detected anti-HlyE responses at the time of clinical presentation in patients but not in controls. These findings could assist in the development of improved diagnostic assays.
机译:伤寒沙门氏菌导致的原因伤寒和human-restricted病原体。目前伤寒疫苗提供5090%保护2到5年,可用实际诊断化验确定伤寒患者缺乏敏感性和/或特异性。在人类感染伤寒抗原表达可能导致改进诊断化验吗疫苗。immunoaffinity proteomics-based技术(IPT)包括列控的使用抗体IgG、IgM或IgA分数恢复从人类与伤寒杆菌bacteremic捕获随后的伤寒杆菌蛋白质质谱法鉴定。确定免疫原性的蛋白质识别的工具通过抗体从受感染的主机。技术和患者的血浆。伤寒菌血症在孟加拉国,我们确定了57伤寒杆菌的蛋白质,包括已知的蛋白质免疫原性(PagC, HlyE、OmpA GroEL)大量的蛋白质中human-restricted伤寒血清型S和S。甲型副伤寒但很少发现broader-host-range沙门氏菌spp。(HlyE CdtB,PltA, STY1364)。一些主要的蛋白质组,包括那些参与能量代谢,蛋白质合成,铁内稳态,而这些生物合成和代谢功能预测本地化外膜。评估系统和粘膜anti-HlyE响应在美国Typhi-infected患者和检测anti-HlyE临床时的反应表现在病人而不是控制。这些发现可能帮助发展的改进诊断化验。

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