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首页> 外文期刊>BMC Microbiology >Effect of deletion of gene cluster involved in synthesis of Enterobacterial common antigen on virulence and immunogenicity of live attenuated Salmonella vaccine when delivering heterologous Streptococcus pneumoniae antigen PspA
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Effect of deletion of gene cluster involved in synthesis of Enterobacterial common antigen on virulence and immunogenicity of live attenuated Salmonella vaccine when delivering heterologous Streptococcus pneumoniae antigen PspA

机译:基因簇缺失在递送异源链球菌抗原PSPA时缺乏肠杆菌常见抗原合成对肠杆菌常见抗原的毒力和免疫原性的影响

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Enterobacterial common antigen (ECA) is a family-specific surface antigen shared by all members of the Enterobacteriaceae family. Previous studies showed that the loss of ECA results in Salmonella attenuation, indicating its usefulness as a vaccine candidate for Salmonella infection, but no studies have shown whether the mutation resulting from the deletion of the ECA operon in conjunction with other mutations could be used as an antigen vehicle for heterologous protein antigen delivery. In this study, we introduced a nonpolar, defined ECA operon deletion into wild-type S. Typhimurium χ3761 and an attenuated vaccine strain χ9241, obtaining two isogenic ECA operon mutants, namely, χ12357 and χ12358, respectively. A number of in vitro and in vivo properties of the mutants were analyzed. We found that the loss of ECA did not affect the growth, lipopolysaccharide (LPS) production and motility of S. Typhimurium wild type strain χ3761 and its attenuated vaccine strain χ9241 but significantly affected the virulence when administered orally to BALB/c mice. Furthermore, the effects of the ECA mutation on the immunogenicity of a recombinant S. Typhimurium vaccine strain χ9241 when delivering the pneumococcal antigen PspA were determined. The result showed that the total anti-PspA IgG level of χ12358 (pYA4088) was slightly lower than that of χ9241 (pYA4088), but the protection rate was not compromised. ECA affects virulence and benefits the Th2 immunity of Salmonella Typhimurium, therefore, it is feasible to use a reversible ECA mutant mode to design future Salmonella vaccine strains for heterologous protective antigens.
机译:细菌常见的抗原(ECA)是由肠杆菌族家族的所有成员共享的家用表面抗原。以前的研究表明,ECA的丧失导致沙门氏菌衰减,表明其作为沙门氏菌感染的疫苗候选者的用途,但没有研究由与其他突变结合删除ECA操纵子导致的突变是可以使用的异源蛋白抗原递送的抗原载体。在这项研究中,我们将非极性定义的ECA操纵子缺失纳入野生型S. typhimuriumχ3761和衰减疫苗菌株χ9241,即分别获得两个等源性ECA操纵子突变体,即χ12357和χ12358。分析了许多体外和突变体的体内性质。我们发现ECA的丧失不影响S.毒鼠野生型菌株χ3761的生长,脂多糖(LPS)生产和动力,其减毒疫苗菌株χ9241,但在口服给Balb / C小鼠时显着影响了毒力。此外,测定了ECA突变对重组​​S.培氏疫苗菌​​株α9241的免疫原性的影响。结果表明,χ12358(PyA4088)的总抗PSPA IgG水平略低于χ9241(PyA4088),但保护率并未受到损害。 ECA影响毒力并益处沙门氏菌的Th2免疫力,因此,使用可逆的ECA突变模式设计用于异源保护抗原的未来沙门氏菌疫苗菌株是可行的。

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