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Characterization of Immunological Cross-Reactivity between Enterotoxigenic Escherichia coli Heat-Stable Toxin and Human Guanylin and Uroguanylin

机译:产肠毒素的大肠杆菌热稳定毒素与人鸟嘌呤和尿鸟苷之间的免疫交叉反应性表征

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Enterotoxigenic Escherichia coli (ETEC) expressing the heat-stable toxin (ST) (human-type [STh] and porcine-type [STp] variants) is among the five most important enteric pathogens in young children living in low- and middle-income countries. ST mediates diarrheal disease through activation of the guanylate cyclase C (GC-C) receptor and is an attractive vaccine target with the potential to confer protection against a wide range of ETEC strains. However, immunological cross-reactivity to the endogenous GC-C ligands guanylin and uroguanylin is a major concern because of the similarities to ST in amino acid sequence, structure, and function. We have investigated the presence of similar epitopes on STh, STp, guanylin, and uroguanylin by analyzing these peptides in eight distinct competitive enzyme-linked immunosorbent assays (ELISAs). A fraction (27%) of a polyclonal anti-STh antibody and an anti-STh monoclonal antibody (MAb) cross-reacted with uroguanylin, the latter with a 73-fold-lower affinity. In contrast, none of the antibodies raised against STp, one polyclonal antibody and three MAbs, cross-reacted with the endogenous peptides. Antibodies raised against guanylin and uroguanylin showed partial cross-reactivity with the ST peptides. Our results demonstrate, for the first time, that immunological cross-reactions between ST and the endogenous peptides can occur. However, the partial nature and low affinity of the observed cross-reactions suggest that the risk of adverse effects from a future ST vaccine may be low. Furthermore, our results suggest that this risk may be reduced or eliminated by basing an ST immunogen on STp or a selectively mutated variant of STh.
机译:表达热稳定毒素(ST)(人型[STh]和猪型[STp]变体)的肠毒素大肠杆菌(ETEC)是生活在中低收入儿童中的五个最重要的肠道病原体之一国家。 ST通过鸟苷酸环化酶C(GC-C)受体的活化介导腹泻病,是一种有吸引力的疫苗靶标,具有针对多种ETEC菌株提供保护的潜力。然而,由于氨基酸序列,结构和功能上与ST相似,与内源GC-C配体鸟苷和尿鸟苷的免疫交叉反应是一个主要问题。我们已经通过在八种不同的竞争性酶联免疫吸附测定(ELISA)中分析这些肽,研究了STh,STp,鸟苷和尿鸟苷上相似表位的存在。一部分(27%)多克隆抗STh抗体和抗STh单克隆抗体(MAb)与尿鸟苷素交叉反应,后者的亲和力低73倍。相反,没有一种抗STp的抗体,一种多克隆抗体和三种MAb与内源肽发生交叉反应。针对鸟苷蛋白和尿鸟苷蛋白的抗体显示出与ST肽的部分交叉反应性。我们的结果首次证明,ST和内源性肽之间可能发生免疫交叉反应。但是,观察到的交叉反应的部分性质和低亲和力表明,未来ST疫苗产生不良反应的风险可能较低。此外,我们的结果表明,通过将ST免疫原置于STp或STh的选择性突变变体上,可以降低或消除这种风险。

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