Bacterial copper- and zinc-cofactored superoxide dismutase contributes to the pathogenesis of systemic salmonellosis |
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Authors: | Jayne L. Farrant,Assunta Sansone,James R. Canvin,Mark J. Pallen,Paul R. Langford,Timothy S. Wallis,Gordon Dougan,& J. Simon Kroll |
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Affiliation: | Molecular Infectious Diseases Group, Department of Paediatrics, Imperial College School of Medicine at St Mary's, Norfolk Place, London W2 1PG, UK.,;Institute for Animal Health, Compton, Newbury RG20 0NN, UK.,;Department of Biochemistry, Imperial College of Science, Technology and Medicine, London SW7 2AZ, UK. |
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Abstract: | ![]() Copper/zinc-cofactored superoxide dismutase ([Cu,Zn]-SOD) has been found in the periplasm of many bacterial species but its biological function is unknown. Here we report the cloning and characterization of sodC , encoding [Cu,Zn]-SOD, from Salmonella typhimurium . The predicted protein sequence shows only 58% identity to Escherichia coli SodC, and from this its chromosomal location and its immediate proximity to a phage gene, sodC , in Salmonella is speculated to have been acquired by bacteriophage-mediated horizontal transfer from an unknown donor. A sodC mutant of S . typhimurium was unimpaired on aerobic growth in rich medium but showed enhanced sensitivity in vitro to the microbicidal action of superoxide. S . typhimurium , S . choleraesuis and S . dublin sodC mutants showed reduced lethality in a mouse model of oral infection and persisted in significantly lower numbers in livers and spleens after intraperitoneal infection, suggesting that [Cu,Zn]-SOD plays a role in pathogenicity, protecting Salmonella against oxygen radical-mediated host defences. There was, however, no observable difference compared with wild type in the interaction of sodC mutants with porcine pleural, mouse peritoneal or J774 macrophages in vitro , perhaps reflecting the hierarchical capacity of different macrophage lines to kill Salmonella , the most efficient overwhelming the proposed protective effect of periplasmic SOD. |
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