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Robust immune response elicited by a novel and unique Mycobacterium tuberculosis protein using an optimized DNA/protein heterologous prime/boost protocol

机译:新型和独特的结核分枝杆菌蛋白质使用优化的DNA /蛋白质异源引发/增强方案引发的强大免疫应答

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摘要

An efficacious tuberculosis (TB) vaccine will probably need to induce both CD4 and CD8 T-cell responses specific to a protective Mycobacterium tuberculosis antigen(s). To achieve this broad cellular immune response we tested a heterologous DNA/protein combination vaccine strategy. We used a purified recombinant protein preparation of a unique M. tuberculosis antigen (rMT1721) found in the urine of TB patients, an optimized plasmid DNA expressing this protein (DNA-MT1721), and a Toll-like receptor 4 agonist adjuvant. We found that priming mice with DNA-MT1721 and subsequently boosting with rMT1721 elicited high titres of specific IgG1 and IgG2a antibodies as well as high magnitude and polyfunctional CD4+ T-cell responses. However, no detectable CD8+ T-cell response was observed using this regimen of immunization. In contrast, both CD4+ and CD8+ T-cell responses were detected after a prime/boost vaccination regimen using rMT1721 as the priming antigen and DNA-MT1721 as the boosting immunogen. These findings support the exploration of heterologous DNA/protein immunization strategies in vaccine development against TB and possibly other infectious diseases.
机译:有效的肺结核(TB)疫苗可能需要诱导对保护性结核分枝杆菌抗原具有特异性的CD4和CD8 T细胞反应。为了实现这种广泛的细胞免疫应答,我们测试了异源DNA /蛋白质组合疫苗策略。我们使用了在结核病患者尿液中发现的独特结核分枝杆菌抗原(rMT1721)的纯化重组蛋白制剂,表达该蛋白的优化质粒DNA(DNA-MT1721)和Toll样受体4激动剂佐剂。我们发现,用DNA-MT1721引发小鼠并随后用rMT1721加强免疫可引起高滴度的特异性IgG1和IgG2a抗体,以及高强度和多功能CD4 + T细胞反应。但是,使用这种免疫方案没有观察到可检测的CD8 + T细胞应答。相反,在使用rMT1721作为初次抗原和DNA-MT1721作为加强免疫原的初次/加强疫苗接种方案后,检测到CD4 + 和CD8 + T细胞反应。这些发现支持在针对结核病和可能其他传染病的疫苗开发中探索异源DNA /蛋白质免疫策略。

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