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重组 CS6 衍生亚单位肠毒素性大肠杆菌候选疫苗的生化和免疫评估。

Biochemical and Immunological Evaluation of Recombinant CS6-Derived Subunit Enterotoxigenic Escherichia coli Vaccine Candidates.

机构信息

Henry M. Jackson Foundation for the Advancement of Military Medicine, Bethesda, Maryland, USA

Department of Microbiology and Immunology, Uniformed Services University of the Health Sciences, Bethesda, Maryland, USA.

出版信息

Infect Immun. 2019 Feb 21;87(3). doi: 10.1128/IAI.00788-18. Print 2019 Mar.

Abstract

CS6, a prevalent surface antigen expressed in nearly 20% of clinical enterotoxigenic (ETEC) isolates, is comprised of two major subunit proteins, CssA and CssB. Using donor strand complementation, we constructed a panel of recombinant proteins of 1 to 3 subunits that contained combinations of CssA and/or CssB subunits and a donor strand, a C-terminal extension of 16 amino acids that was derived from the N terminus of either CssA or CssB. While the entire panel of recombinant proteins could be obtained as soluble, folded proteins, it was observed that the proteins possessing a heterologous donor strand, derived from the CS6 subunit different from the C-terminal subunit, had the highest degree of physical and thermal stability. Immunological characterization of the proteins, using a murine model, demonstrated that robust anti-CS6 immune responses were generated from fusions containing both CssA and CssB. Proteins containing only CssA were weakly immunogenic. Heterodimers, i.e., CssBA and CssAB, were sufficient to recapitulate the anti-CS6 immune response elicited by immunization with CS6, including the generation of functional neutralizing antibodies, as no further enhancement of the response was obtained with the addition of a third CS6 subunit. Our findings here demonstrate the feasibility of including a recombinant CS6 subunit protein in a subunit vaccine strategy against ETEC.

摘要

CS6 是一种在近 20%的临床肠产毒性(ETEC)分离株中表达的流行表面抗原,由两个主要亚基蛋白 CssA 和 CssB 组成。通过供体链互补,我们构建了一组包含 1 到 3 个亚基的重组蛋白,这些亚基包含 CssA 和/或 CssB 亚基和供体链的组合,供体链是源自 CssA 或 CssB N 端的 16 个氨基酸的 C 末端延伸。虽然整个重组蛋白组都可以作为可溶的、折叠的蛋白质获得,但观察到具有异源供体链的蛋白质,其源自与 C 末端亚基不同的 CS6 亚基,具有最高的物理和热稳定性。使用小鼠模型对蛋白质进行免疫特性分析表明,来自包含 CssA 和 CssB 的融合物的强抗 CS6 免疫反应被产生。仅包含 CssA 的蛋白质的免疫原性较弱。异二聚体,即 CssBA 和 CssAB,足以重现用 CS6 免疫引发的抗 CS6 免疫反应,包括产生功能性中和抗体,因为添加第三个 CS6 亚基不会进一步增强反应。我们在这里的发现证明了在针对 ETEC 的亚单位疫苗策略中包含重组 CS6 亚单位蛋白的可行性。

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