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Capsular polysaccharide-protein conjugate vaccines of carbotype 1 Vibrio vulnificus: construction immunogenicity and protective efficacy in a murine model.

机译:Carbotype 1创伤弧菌的荚膜多糖-蛋白质结合疫苗:在鼠模型中的构建免疫原性和保护功效。

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摘要

Vibrio vulnificus causes septicemia and wound infections in immunocompromised humans. The capsular polysaccharide of Vibrio vulnificus (VvPS) is critical for virulence. We synthesized conjugate vaccines of carbotype 1 VvPS under conditions and in formulations suitable for human use. Purified VvPS was conjugated to tetanus toxoid (TT) or to inactivated V. vulnificus cytolysin or elastase by two different schemes. All conjugates elicited elevated anticapsular immunoglobulin G (IgG) and IgM and antiprotein IgG responses in mice compared with saline placebo. The conjugates prepared through caboxyl activation of VvPS (VvPS-TTa, VvPS-cytolysin, and VvPS-elastase) were more immunogenic than the one prepared through hydroxyl activation (VvPS-TTb). The protective efficacy of conjugated and unconjugated formulations of VvPS and that of protein carriers were evaluated in a mouse septicemia model. Eighty percent of mice actively immunized with VvPS-TTa vaccine survived challenge with carbotype 1 V. vulnificus, while VvPS-cytolysin and VvPS-elastase conjugates conferred 44 and 40% protection, respectively. Control mice immunized with VvPS, cytolysin, or elastase alone, or saline only, showed 70 to 100% mortality. VvPS-TTa vaccine is nontoxic, immunogenic, and protective in mice.
机译:创伤弧菌会导致免疫力低下的人败血症和伤口感染。创伤弧菌荚膜多糖(VvPS)对毒力至关重要。我们在适合人类使用的条件下和配方中合成了1型vvPS的结合疫苗。通过两种不同的方法,将纯化的VvPS与破伤风类毒素(TT)或灭活的创伤弧菌溶血素或弹性蛋白酶偶联。与盐水安慰剂相比,所有缀合物在小鼠中引起升高的抗荚膜免疫球蛋白G(IgG)和IgM和抗蛋白IgG应答。通过VvPS的羧基活化制备的结合物(VvPS-TTa,VvPS-细胞溶素和VvPS-弹性蛋白酶)比通过羟基活化制备的结合物(VvPS-TTb)更具免疫原性。在小鼠败血病模型中评估了VvPS偶联和未偶联制剂的保护功效以及蛋白载体的防护功效。用VvPS-TTa疫苗主动免疫的小鼠中有80%在1型碳弧菌中存活下来,而VvPS-溶血素和VvPS-弹性蛋白酶偶联物分别提供了44%和40%的保护。仅用VvPS,溶细胞素或弹性蛋白酶或仅用生理盐水免疫的对照小鼠显示70至100%的死亡率。 VvPS-TTa疫苗对小鼠无毒,具有免疫原性和保护性。

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