SecA2 functions in the secretion of superoxide dismutase A and in the virulence of Mycobacterium tuberculosis

M Braunstein, BJ Espinosa, J Chan… - Molecular …, 2003 - Wiley Online Library
M Braunstein, BJ Espinosa, J Chan, JT Belisle, W R. Jacobs Jr
Molecular microbiology, 2003Wiley Online Library
Tuberculosis remains a severe worldwide health threat. A thorough understanding of
Mycobacterium tuberculosis pathogenesis will facilitate the development of new treatments
for tuberculosis. Numerous bacterial pathogens possess specialized protein secretion
systems that are dedicated to the export of virulence factors. Mycobacterium tuberculosis is
part of a developing group of pathogenic bacteria that share the uncommon property of
possessing two secA genes (secA1 and secA2). In mycobacteria, SecA1 is the essential …
Summary
Tuberculosis remains a severe worldwide health threat. A thorough understanding of Mycobacterium tuberculosis pathogenesis will facilitate the development of new treatments for tuberculosis. Numerous bacterial pathogens possess specialized protein secretion systems that are dedicated to the export of virulence factors. Mycobacterium tuberculosis is part of a developing group of pathogenic bacteria that share the uncommon property of possessing two secA genes (secA1 and secA2). In mycobacteria, SecA1 is the essential ‘housekeeping’ SecA protein whereas SecA2 is an accessory secretion factor. Here we demonstrate that SecA2 contributes to the pathogenesis of M. tuberculosis. A deletion of the secA2 gene in M. tuberculosis attenuates the virulence of the organism in mice. By comparing the profile of proteins secreted by wild‐type M. tuberculosis and the ΔsecA2 mutant, we identified superoxide dismutase A (SodA) as a protein dependent on SecA2 for secretion. SodA lacks a classical signal sequence for protein export. Our data suggests that SecA2‐dependent export is a new type of secretion pathway that is part of a virulence mechanism of M. tuberculosis to elude the oxidative attack of macrophages.
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