首页> 美国卫生研究院文献>Clinical and Diagnostic Laboratory Immunology >Multiepitope Fusion Antigen Induces Broadly Protective Antibodies That Prevent Adherence of Escherichia coli Strains Expressing Colonization Factor Antigen I (CFA/I) CFA/II and CFA/IV
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Multiepitope Fusion Antigen Induces Broadly Protective Antibodies That Prevent Adherence of Escherichia coli Strains Expressing Colonization Factor Antigen I (CFA/I) CFA/II and CFA/IV

机译:多表位融合抗原诱导广泛的保护性抗体可防止表达定殖因子抗原I(CFA / I)CFA / II和CFA / IV的大肠杆菌菌株的粘附

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摘要

Diarrhea is the second leading cause of death in children younger than 5 years and continues to be a major threat to global health. Enterotoxigenic Escherichia coli (ETEC) strains are the most common bacteria causing diarrhea in developing countries. ETEC strains are able to attach to host small intestinal epithelial cells by using bacterial colonization factor antigen (CFA) adhesins. This attachment helps to initiate the diarrheal disease. Vaccines that induce antiadhesin immunity to block adherence of ETEC strains that express immunologically heterogeneous CFA adhesins are expected to protect against ETEC diarrhea. In this study, we created a CFA multiepitope fusion antigen (MEFA) carrying representative epitopes of CFA/I, CFA/II (CS1, CS2, and CS3), and CFA/IV (CS4, CS5, and CS6), examined its immunogenicity in mice, and assessed the potential of this MEFA as an antiadhesin vaccine against ETEC. Mice intraperitoneally immunized with this CFA MEFA exhibited no adverse effects and developed immune responses to CFA/I, CFA/II, and CFA/IV adhesins. Moreover, after incubation with serum of the immunized mice, ETEC or E. coli strains expressing CFA/I, CFA/II, or CFA/IV adhesins were significantly inhibited in adherence to Caco-2 cells. Our results indicated this CFA MEFA elicited antibodies that not only cross-reacted to CFA/I, CFA/II and CFA/IV adhesins but also broadly inhibited adherence of E. coli strains expressing these seven adhesins and suggested that this CFA MEFA could be a candidate to induce broad-spectrum antiadhesin protection against ETEC diarrhea. Additionally, this antigen construction approach (creating an MEFA) may be generally used in vaccine development against heterogenic pathogens.
机译:腹泻是5岁以下儿童的第二大死亡原因,并且仍然是对全球健康的主要威胁。产肠毒素的大肠杆菌(ETEC)菌株是发展中国家引起腹泻的最常见细菌。 ETEC菌株能够通过使用细菌定殖因子抗原(CFA)粘附素附着在宿主小肠上皮细胞上。这种附件有助于引发腹泻病。诱导抗粘附素免疫以阻止表达免疫学上异源的CFA粘附素的ETEC菌株粘附的疫苗有望预防ETEC腹泻。在这项研究中,我们创建了一个带有CFA / I,CFA / II(CS1,CS2和CS3)和CFA / IV(CS4,CS5和CS6)代表性表位的CFA多表位融合抗原(MEFA),并检查了其免疫原性并评估了这种MEFA作为抗ETEC的抗粘附素疫苗的潜力。用这种CFA MEFA腹膜内免疫的小鼠没有不良反应,并且对CFA / I,CFA / II和CFA / IV粘附素产生了免疫应答。而且,在与免疫小鼠的血清一起温育后,表达CFA / I,CFA / II或CFA / IV粘附素的ETEC或大肠杆菌菌株显着抑制了对Caco-2细胞的粘附。我们的结果表明,这种CFA MEFA引发的抗体不仅与CFA / I,CFA / II和CFA / IV黏附素发生交叉反应,而且还广泛抑制表达这7种黏附素的大肠杆菌菌株的粘附,这表明该CFA MEFA可能是一种诱导广谱抗粘附素抵抗ETEC腹泻的候选药物。此外,这种抗原构建方法(创建MEFA)通常可用于针对异源病原体的疫苗开发中。

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