Article ID | Journal | Published Year | Pages | File Type |
---|---|---|---|---|
8485345 | Tuberculosis | 2016 | 14 Pages |
Abstract
Mycobacterium tuberculosis (Mtb) survives inside the macrophages by modulating the host immune responses in its favor. The 6-kDa early secretory antigenic target (ESAT-6; esxA) of Mtb is known as a potent virulence and T-cell antigenic determinant. At least 23 such ESAT-6 family proteins are encoded in the genome of Mtb; however, the function of many of them is still unknown. We herein report that ectopic expression of Mtb Rv2346c (esxO), a member of ESAT-6 family proteins, in non-pathogenic Mycobacterium smegmatis strain (MsmRv2346c) aids host cell invasion and intracellular bacillary persistence. Further mechanistic studies revealed that MsmRv2346c infection abated macrophage immunity by inducing host cell death and genomic instability as evident from the appearance of several DNA damage markers. We further report that the induction of genomic instability in infected cells was due to increase in the hosts oxidative stress responses. MsmRv2346c infection was also found to induce autophagy and modulate the immune function of macrophages. In contrast, blockade of Rv2346c induced oxidative stress by treatment with ROS inhibitor N-acetyl-L-cysteine prevented the host cell death, autophagy induction and genomic instability in infected macrophages. Conversely, MtbÎRv2346c mutant did not show any difference in intracellular survival and oxidative stress responses. We envision that Mtb ESAT-6 family protein Rv2346c dampens antibacterial effector functions namely by inducing oxidative stress mediated genomic instability in infected macrophages, while loss of Rv2346c gene function may be compensated by other redundant ESAT-6 family proteins. Thus EsxO plays an important role in mycobacterial pathogenesis in the context of innate immunity.
Keywords
O.DIL-12PCDNF-κBMTBIL-10MSMCFURNSiNOSNACFBSMycobacterium smegmatis3-(4,5-dimethylthiazol-2-yl)-2,5-diphenyltetrazolium bromideMOIMTTROSInterleukin 10interleukin 12SurvivalGenomic instabilityOxidative stresstumor necrosis factor alphaSODfetal bovine seruminducible nitric oxide synthaseSuperoxide dismutaseTNF-αMacrophagesMycobacterium tuberculosisProgrammed cell deathwild typeNitric oxideN-acetyl cysteinemultiplicity of infectionoptical densitycolony forming unitreactive nitrogen speciesReactive oxygen species
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Authors
Soumitra Mohanty, Michael Dal Molin, Geetanjali Ganguli, Avinash Padhi, Prajna Jena, Petra Selchow, Srabasti Sengupta, Michael Meuli, Peter Sander, Avinash Sonawane,