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首页> 外文期刊>Cell Reports >Recombinant BCG Expressing ESX-1 of Mycobacterium marinum Combines Low Virulence with Cytosolic Immune Signaling and Improved TB Protection
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Recombinant BCG Expressing ESX-1 of Mycobacterium marinum Combines Low Virulence with Cytosolic Immune Signaling and Improved TB Protection

机译:表达海洋分枝杆菌ESX-1的重组卡介苗结合了低毒力和胞质免疫信号,并改善了结核病的保护

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Recent insights into the mechanisms by which Mycobacterium tuberculosis, the etiologic agent of human tuberculosis, is recognized by cytosolic nucleotide sensors have opened new avenues for rational vaccine design. The only licensed anti-tuberculosis vaccine, Mycobacterium bovis BCG, provides limited protection. A feature of BCG is the partial deletion of the ESX-1 type VII secretion system, which governs phagosomal rupture and cytosolic pattern recognition, key intracellular phenotypes linked to increased immune signaling. Here, by heterologously expressing the esx-1 region of Mycobacterium marinum in BCG, we engineered a low-virulence, ESX-1-proficient, recombinant BCG (BCG::ESX-1^M^m^a^r) that induces the cGas/STING/TBK1/IRF-3/type I interferon axis and enhances AIM2 and NLRP3 inflammasome activity, resulting in both higher proportions of CD8^+ T cell effectors against mycobacterial antigens shared with BCG and polyfunctional CD4^+ Th1 cells specific to ESX-1 antigens. Importantly, independent mouse vaccination models show that BCG::ESX-1^M^m^a^r confers superior protection relative to parental BCG against challenges with highly virulent M. tuberculosis.
机译:人们对结核分枝杆菌(人类结核病的病原体)被胞质核苷酸传感器识别的机理的最新见解为合理的疫苗设计开辟了新途径。唯一获得许可的抗结核疫苗牛分枝杆菌BCG提供有限的保护。 BCG的一个特征是ESX-1 VII型分泌系统的部分缺失,该系统控制吞噬体破裂和胞浆模式识别,这些关键细胞内表型与增加的免疫信号传导有关。在这里,我们通过在BCG中异源表达海洋分枝杆菌的esx-1区,我们设计了一种低毒力,ESX-1高效的重组BCG(BCG :: ESX-1 ^ M ^ m ^ a ^ r), cGas / STING / TBK1 / IRF-3 / I型干扰素轴并增强AIM2和NLRP3炎性体活性,导致针对与BCG共享的分枝杆菌抗原的CD8 ^ + T细胞效应子和针对ESX的多功能CD4 ^ + Th1细胞的比例更高-1抗原。重要的是,独立的小鼠疫苗接种模型表明BCG :: ESX-1 ^ M ^ m ^ a ^ r相对于亲本BCG赋予了抵抗高毒结核分枝杆菌挑战的优越保护。

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