@article{open3312,
          volume = {15},
          number = {1},
           month = {June},
          author = {Tannu Priya Gosain and Saurabh Chugh and Zaigham Abbas Rizvi and Neeraj Kumar Chauhan and Saqib Kidwai and Krishan Gopal Thakur and Amit Awasthi and Ramandeep Singh},
           title = {Mycobacterium tuberculosis strain with deletions in menT3 and menT4 is attenuated and confers protection in mice and guinea pigs},
       publisher = {Springer Science and Business Media LLC},
            year = {2024},
         journal = {Nat. Commun.},
           pages = {5467},
             url = {http://crdd.osdd.net/open/3312/},
        abstract = {The genome of Mycobacterium tuberculosis encodes for a large repertoire of toxin-antitoxin systems. In the present study, MenT3 and MenT4 toxins belonging to MenAT subfamily of TA systems have been functionally characterized. We demonstrate that ectopic expression of these toxins inhibits bacterial growth and this is rescued upon co-expression of their cognate antitoxins. Here, we show that simultaneous deletion of menT3 and menT4 results in enhanced susceptibility of M. tuberculosis upon exposure to oxidative stress and attenuated growth in guinea pigs and mice. We observed reduced expression of transcripts encoding for proteins that are essential or required for intracellular growth in mid-log phase cultures of {\ensuremath{\Delta}}menT4{\ensuremath{\Delta}}T3 compared to parental strain. Further, the transcript levels of proteins involved in efficient bacterial clearance were increased in lung tissues of {\ensuremath{\Delta}}menT4{\ensuremath{\Delta}}T3 infected mice relative to parental strain infected mice. We show that immunization of mice and guinea pigs with {\ensuremath{\Delta}}menT4{\ensuremath{\Delta}}T3 confers significant protection against M. tuberculosis infection. Remarkably, immunization of mice with {\ensuremath{\Delta}}menT4{\ensuremath{\Delta}}T3 results in increased antigen-specific TH1 bias and activated memory T cell response. We conclude that MenT3 and MenT4 are important for M. tuberculosis pathogenicity and strains lacking menT3 and menT4 have the potential to be explored further as vaccine candidates.}
}