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Protection of pigs against Taenia solium cysticercosis using recombinant antigen or in combination with DNA vaccine

机译:重组抗原或与DNA疫苗联合使用可保护猪免于感染猪带状Ta虫

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摘要

In the present study, we investigated the duration of protection afforded to pigs immunized in two different prime-boost regimens: one is homologus priming and boosting with a protein vaccine, and the other is priming with a DNA vaccine and boosting with the protein vaccine. Groups of pigs that received the same vaccination regimen were then challenged with Taenia solium eggs at 6, 12 or 20 weeks post-immunization (wpi), respectively. The results showed that all vaccinated pigs challenged at 6 or 12 wpi showed significant (P < 0.05) reduction in the development of cysts. When challenged at 20 wpi, pigs primed with the DNA vaccine (pcDNA3-cC1) followed by two boosters of the protein vaccine (GST-cC1) showed significant (P < 0.05) protection against the challenge of T solium eggs, whereas pigs receiving three injections of the protein vaccine showed no significant protection compared to non-vaccinated controls (P > 0.05). Antibody isotype assays showed that DNA prime-protein boost regimen induced a predominantly IgG2 response, compared to an IgG1 biased response for the protein prime-protein boost regimen. In addition, peripheral blood mononuclear cells (PBMC) obtained from the DNA prime-protein boost group proliferated strongly in response to GST-cC1 protein, and this responsiveness persisted until 20 wpi. Taken together, our data suggest that the use of a prime-boost strategy combining DNA and protein vaccines may be better than protein alone for the longevity of protection against the challenge of T solium eggs.
机译:在本研究中,我们调查了在两种不同的初免-加强方案中对猪免疫的保护时间:一种是同源疫苗和蛋白质疫苗加强免疫,另一种是DNA疫苗和蛋白质疫苗加强免疫。然后在免疫后第6、12或20周分别用Taenia lium虫卵对接受相同疫苗接种方案的猪群进行攻击。结果表明,所有在6或12 wpi时接种的疫苗接种猪的囊肿发育均显着(P <0.05)降低。当以20 wpi的剂量攻击时,先用DNA疫苗(pcDNA3-cC1)进行免疫,然后再用两次蛋白疫苗加强免疫(GST-cC1)的猪对T eggs虫卵的攻击表现出显着(P <0.05)的保护作用,而接受三只T卵的猪则受到保护与未接种疫苗的对照组相比,注射蛋白疫苗没有显示出明显的保护作用(P> 0.05)。抗体同种型分析表明,与蛋白质主要蛋白质增强方案的IgG1偏倚反应相比,DNA优质蛋白质增强方案主要诱发IgG2应答。此外,从DNA初级蛋白质增强组获得的外周血单核细胞(PBMC)强烈响应GST-cC1蛋白增殖,并且这种响应性一直持续到20 wpi。综上所述,我们的数据表明,结合使用DNA和蛋白质疫苗的初免-加强策略可能比单独使用蛋白质更好,因为它能长期抵抗T lium虫卵的攻击。

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