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首页> 外文期刊>Vaccine >Immunization of BALB/c mice with a combination of four recombinant Brucella abortus proteins, AspC, Dps, InpB and Ndk, confers a marked protection against a virulent strain of Brucella abortus
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Immunization of BALB/c mice with a combination of four recombinant Brucella abortus proteins, AspC, Dps, InpB and Ndk, confers a marked protection against a virulent strain of Brucella abortus

机译:BALB / C小鼠的免疫组合具有四个重组布鲁氏菌毒物蛋白,ASPC,DPS,INPB和NDK的组合赋予了对Brucella Abortus的毒性菌株的显着保护

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In this study, we assessed the protective efficacy of single subunit vaccines, encoded by the B. abortus 544 genes aspC, dps, yaeC and inpB, against B. abortus infection in mice. First, immunization with these antigens, with the exception of the YaeC protein, was found to elicit both humoral and cellular immune responses with IgG2a being dominant over IgG1. In addition, a massive production of 1FN-gamma but lower degree of IL-10 was observed, suggesting that all three antigens were able to induce predominantly cell-mediated immunity in response to B. abortus infection. Further investigation of a combined subunit vaccine (CSV) consisting of purified AspC, Dps, InpB and Ndk proteins showed a superior protective effect in mice against brucellosis. The intraperitoneal injection of this combination was shown to induce a remarkable production of IFN-gamma and IL-2, which occurred in conjunction with an increase of blood CD4(+) and CD8(+) T cell proportions. In addition, the higher titer of IgG2a compared to IgG1 elicited by this CSV was obtained, suggesting that this CSV induced a typical T-helper-1 -dominated immune response in vivo. Furthermore, the protection level induced by this combination was significantly higher than that induced by single antigens and was not significantly different compared to a group immunized with a live attenuated vaccine (RB51). Altogether, our findings suggest that the combination of different immunogenic antigens could be a useful approach for the development of a new, effective and safe brucellosis vaccine that can replace current vaccine strains. (C) 2018 Elsevier Ltd. All rights reserved.
机译:在这项研究中,我们评估了由B. abortius 544基因Aspc,Dps,yaec和Inpb编码的单次亚基疫苗的保护效果对小鼠的B. abortius感染。首先,发现与yaec蛋白外,用这些抗原免疫,发现与IgG2a占IgG1的IgG2a,引发体液和细胞免疫应答。此外,观察到大量生产的1Fn-gamma但较低程度的IL-10,表明所有三种抗原能够响应B. Abortus感染响应B. Abortius感染而主要诱导细胞介导的免疫。进一步研究由纯化的ASPC,DPS,INPB和NDK蛋白组成的组合亚基疫苗(CSV),对小鼠抵抗布鲁氏症的优异保护作用。显示这种组合的腹腔注射诱导IFN-Gamma和IL-2的显着产生,其结合增加血液CD4(+)和CD8(+)T细胞比例。另外,获得与通过该CSV引发的IgG1相比的IgG2a的较高滴度,表明该CSV在体内诱导了典型的T-辅助-1-adminated免疫应答。此外,与用活化疫苗(RB51)免疫的组相比,这种组合诱导的保护水平显着高于单抗原诱导的保护水平,并且与免疫的基团没有显着差异(RB51)。我们的研究结果表明,不同免疫原性抗原的组合可以是开发一种可以取代目前疫苗菌株的新型,有效和安全的布鲁氏疫苗的有用方法。 (c)2018年elestvier有限公司保留所有权利。

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