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首页> 外文期刊>Molecular Immunology >Vaccination with recombinant L7/L12-truncated Omp31 protein induces protection against Brucella infection in BALB/c mice
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Vaccination with recombinant L7/L12-truncated Omp31 protein induces protection against Brucella infection in BALB/c mice

机译:用重组L7 / L12截短的Omp31蛋白进行疫苗接种可诱导BALB / c小鼠免受布鲁氏菌感染

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摘要

Brucellosis is the most common bacterial zoonotic disease worldwide and no vaccine is available for the prevention of human brucellosis. In humans, brucellosis is mostly caused by Brucella melitensis and Brucella abortus. The Outer membrane protein 31 (Omp31) and L7/L12 are immunodominant and protective antigens conserved in human Brucella pathogens. In the present study, we evaluated the humoral and cellular immune responses induced by a fusion protein designed based on the Truncated form of Omp31 (TOmp31) and L7-L12 antigens. Vaccination of BALB/c mice with the recombinant fusion protein (rL7/L12-TOmp31) provided the significant protection level against B. melitensis and B. abortus challenge. Moreover, rL7/L12-TOmp31 elicited a strong specific IgG response (higher IgG2a titers) and significant IFN-gamma/IL2 production and T-cell proliferation was also observed. The T helper1 (Th1) oriented response persisted for 12 weeks after the first immunization. The rL7/L12-TOmp31 could be a new potential antigen candidate for the development of a subunit vaccine against B. melitensis and B. abortus. (C) 2015 Elsevier Ltd. All rights reserved.
机译:布鲁氏菌病是全世界最常见的人畜共患疾病,尚无可预防人类布鲁氏菌病的疫苗。在人类中,布鲁氏菌病主要是由布鲁氏菌和流产布鲁氏菌引起的。外膜蛋白31(Omp31)和L7 / L12是人类布鲁氏菌病原体中保守的免疫优势和保护性抗原。在本研究中,我们评估了由基于截短形式的Omp31(TOmp31)和L7-L12抗原设计的融合蛋白诱导的体液和细胞免疫应答。用重组融合蛋白(rL7 / L12-TOmp31)对BALB / c小鼠进行疫苗接种,可提供针对B. melitensis和B.abortus攻击的重要保护水平。此外,rL7 / L12-TOmp31引起强烈的特异性IgG反应(更高的IgG2a滴度),并且还观察到了明显的IFN-γ/ IL2产生和T细胞增殖。首次免疫后,以T helper1(Th1)为导向的应答持续了12周。 rL7 / L12-TOmp31可能是新的潜在抗原候选物,可用于开发抗梅毒双歧杆菌和流产双歧杆菌的亚单位疫苗。 (C)2015 Elsevier Ltd.保留所有权利。

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