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首页> 外文期刊>Clinical & developmental immunology. >Multiple Roles of Myd88 in the Immune Response to the Plague F1-V Vaccine and in Protection against an Aerosol Challenge of Yersinia pestis CO92 in Mice
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Multiple Roles of Myd88 in the Immune Response to the Plague F1-V Vaccine and in Protection against an Aerosol Challenge of Yersinia pestis CO92 in Mice

机译:MyD88在瘟疫F1-V疫苗的免疫反应中的多种作用以及保护Yersinia Pestis Co92在小鼠中的气溶胶挑战

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The current candidate vaccine against Yersinia pestis infection consists of two subunit proteins: the capsule protein or F1 protein and the low calcium response V protein or V-antigen. Little is known of the recognition of the vaccine by the host's innate immune system and how it affects the acquired immune response to the vaccine. Thus, we vaccinated Toll-like receptor (Tlr) 2 , 4 , and 2/4 -double deficient, as well as signal adaptor protein Myd88 -deficient mice. We found that Tlr4 and Myd88 appeared to be required for an optimal immune response to the F1-V vaccine but not Tlr2 when compared to wild-type mice. However, there was a difference between the requirement for Tlr4 and MyD88 in vaccinated animals. When F1-V vaccinated Tlr4 mutant (lipopolysaccharide tolerant) and Myd88 -deficient mice were challenged by aerosol with Y. pestis CO92, all but one Tlr4 mutant mice survived the challenge, but no vaccinated Myd88 -deficient mice survived the challenge. Spleens from these latter nonsurviving mice showed that Y. pestis was not cleared from the infected mice. Our results suggest that MyD88 appears to be important for both an optimal immune response to F1-V and in protection against a lethal challenge of Y. pestis CO92 in F1-V vaccinated mice.
机译:目前对yersinia pestis感染的候选疫苗由两个亚基蛋白质组成:胶囊蛋白或F1蛋白和低钙响应v蛋白或V-antigen。众所周知,宿主的先天免疫系统识别疫苗以及它如何影响对疫苗的获得性免疫应答。因此,我们接种疫苗的受体(TLR)2,4和2/4 - 双缺乏,以及信号适配器蛋白质MyD88的小鼠。我们发现与野生型小鼠相比,对F1-V疫苗的最佳免疫应答的最佳免疫应答,似乎是似乎需要的TLR4和MYD88。然而,在接种疫苗的动物中的TLR4和MYD88的要求之间存在差异。当F1-V接种疫苗的TLR4突变体(脂多糖耐受)和MyD88 - 用Y.Pestis CO92攻击的攻击攻击时,除了一个TLR4突变小鼠的攻击之外,均未在挑战中存活,但没有疫苗的MyD88 -Defice小鼠在挑战中幸存下来。来自这些后者的脾脏的脾脏表明,Y.Pestis未从受感染的小鼠清除。我们的研究结果表明,MyD88对于F1-V对F1-V的最佳免疫应答似乎很重要,并且在F1-V疫苗的小鼠中对Y.Pestis CO92的致死挑战。

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