Center for Tuberculosis Research, Johns Hopkins University School of Medicinegrid.471401.7, Baltimore, Maryland, USA.
VA Portland Health Care System, Portland, Oregon, USA.
mBio. 2021 Feb 22;13(1):e0386521. doi: 10.1128/mbio.03865-21. Epub 2022 Feb 15.
Mucosa-associated invariant T (MAIT) cells play a critical role in antimicrobial defense. Despite increased understanding of their mycobacterial ligands and the clinical association of MAIT cells with tuberculosis (TB), their function in protection against Mycobacterium tuberculosis infection remains unclear. Here, we show that overexpressing key genes of the riboflavin-biosynthetic pathway potentiates MAIT cell activation and results in attenuation of M. tuberculosis virulence . Further, we observed greater control of M. tuberculosis infection in MAIT CAST/EiJ mice than in MAIT C57BL/6J mice, highlighting the protective role of MAIT cells against TB. We also endogenously adjuvanted Mycobacterium bovis BCG with MR1 ligands via overexpression of the lumazine synthase gene and evaluated its protective efficacy in the mouse model of M. tuberculosis infection. Altogether, our findings demonstrate that MAIT cells confer host protection against TB and that overexpression of genes in the riboflavin-biosynthetic pathway attenuates M. tuberculosis virulence. Enhancing MAIT cell-mediated immunity may also offer a novel approach toward improved vaccines against TB. Mucosa-associated invariant T (MAIT) cells are an important subset of innate lymphocytes that recognize microbial ligands derived from the riboflavin biosynthesis pathway and mediate antimicrobial immune responses. Modulated MAIT cell responses have been noted in different forms of tuberculosis. However, it has been unclear if increased MAIT cell abundance is protective against TB disease. In this study, we show that augmentation of the mycobacterial MAIT cell ligands leads to higher MAIT cell activation with reduced M. tuberculosis virulence and that elevated MAIT cell abundance confers greater control of M. tuberculosis infection. Our study also highlights the potential of endogenously adjuvanting the traditional BCG vaccine with MR1 ligands to augment MAIT cell activation. This study increases current knowledge on the roles of the riboflavin-biosynthetic pathway and MAIT cell activation in M. tuberculosis virulence and host immunity against TB.
黏膜相关不变 T (MAIT) 细胞在抗微生物防御中发挥着关键作用。尽管人们对其分枝杆菌配体的理解有所增加,并且 MAIT 细胞与结核病 (TB) 之间存在临床关联,但它们在保护免受结核分枝杆菌感染方面的作用仍不清楚。在这里,我们表明,过度表达核黄素生物合成途径的关键基因可增强 MAIT 细胞的激活,并导致结核分枝杆菌毒力减弱。此外,我们观察到 MAIT CAST/EiJ 小鼠比 MAIT C57BL/6J 小鼠对结核分枝杆菌感染的控制更好,这突出了 MAIT 细胞对结核病的保护作用。我们还通过过表达光氨酸合酶基因将牛分枝杆菌 BCG 与 MR1 配体内源性佐剂化,并在结核分枝杆菌感染的小鼠模型中评估其保护效力。总之,我们的研究结果表明,MAIT 细胞赋予宿主对结核病的保护作用,并且核黄素生物合成途径中的基因过表达可减弱结核分枝杆菌的毒力。增强 MAIT 细胞介导的免疫反应也可能为针对结核病的新型疫苗提供新方法。
黏膜相关不变 T (MAIT) 细胞是先天淋巴细胞的一个重要亚群,它们识别来自核黄素生物合成途径的微生物配体,并介导抗微生物免疫反应。在不同形式的结核病中都注意到 MAIT 细胞反应的调节。然而,增加 MAIT 细胞的丰度是否对结核病疾病具有保护作用尚不清楚。在这项研究中,我们表明,增加分枝杆菌 MAIT 细胞配体可导致更高的 MAIT 细胞激活,结核分枝杆菌毒力降低,并且 MAIT 细胞丰度增加可更好地控制结核分枝杆菌感染。我们的研究还强调了用 MR1 配体内源性佐剂化传统 BCG 疫苗以增强 MAIT 细胞激活的潜力。这项研究增加了关于核黄素生物合成途径和 MAIT 细胞激活在结核分枝杆菌毒力和宿主对结核病的免疫中的作用的现有知识。
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