首页> 外文期刊>The Journal of Veterinary Medical Science >Evaluation of Recombinant Forms of the Shiga Toxin Variant Stx2eB Subunit and Non-Toxic Mutant Stx2e as Vaccine Candidates against Porcine Edema Disease
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Evaluation of Recombinant Forms of the Shiga Toxin Variant Stx2eB Subunit and Non-Toxic Mutant Stx2e as Vaccine Candidates against Porcine Edema Disease

机译:志贺毒素变异Stx2eB亚基和非毒性突变Stx2e重组形式作为猪水肿病疫苗候选者的评价

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References(29) Cited-By(1) Porcine edema disease (ED) is a communicable disease of shoats caused by infection with Shiga toxin (Stx)-producing Escherichia coli. Stx2e is classified as a 1A5B-type toxin and is a decisive virulence determinant of ED. The single A subunit of Stx2e possesses enzymatic activity and is accompanied by a pentamer of B subunits, which binds to the host receptor and delivers the A subunit into the cell. In the present study, we used a mouse model to evaluate the immunogenicity of 3 ED vaccine candidates: a non-toxic mutant holotoxin mStx2e and 2 Stx2eB-based fusion proteins, Stx2eA2B-His and Stx2eB-His. Systemic inoculation of mice with mStx2e- and the Stx2eB-derived antigens induced anti-Stx2e IgG responses that were fully and partially capable of neutralizing Stx2e cellular cytotoxicity, respectively. Intranasal immunization with mStx2e protected the mice from subsequent intraperitoneal challenge with a lethal dose of Stx2e, whereas immunization with Stx2eA2B-His and Stx2eB-His afforded partial protection. Analysis of serum cytokines revealed that mStx2e, but not the Stx2eB-based antigens, was capable of inducing a Th2-type immune response. These results suggest that although the Stx2eB-based antigens elicited an immune response to Stx2e, they did so through a different mechanism to the Th2-type response induced by mStx2e.
机译:参考文献(29)被引用并(1)猪水肿病(ED)是由感染志贺毒素(Stx)的大肠杆菌感染而引起的猪传染病。 Stx2e被分类为1A5B型毒素,是ED的决定性毒力决定因素。 Stx2e的单个A亚基具有酶促活性,并伴有B亚基的五聚体,它与宿主受体结合并将A亚基传递到细胞中。在本研究中,我们使用小鼠模型评估了3种ED疫苗候选者的免疫原性:一种无毒突变体全毒素mStx2e和2种基于Stx2eB的融合蛋白,Stx2eA2B-His和Stx2eB-His。用mStx2e和Stx2eB衍生的抗原对小鼠进行全身接种可诱导抗Stx2e IgG反应,分别完全和部分能够中和Stx2e细胞的细胞毒性。用mStx2e进行鼻内免疫可以用致死剂量的Stx2e保护小鼠免于随后的腹膜内攻击,而用Stx2eA2B-His和Stx2eB-His免疫则可以提供部分保护。血清细胞因子的分析表明,mStx2e,而不是基于Stx2eB的抗原,能够诱导Th2型免疫应答。这些结果表明,尽管基于Stx2eB的抗原引起了对Stx2e的免疫反应,但它们是通过对mStx2e诱导的Th2型反应的机制不同而实现的。

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