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Mycobacterial Esx-3 is required for mycobactin-mediated iron acquisition.


ABSTRACT: The Esx secretion pathway is conserved across Gram-positive bacteria. Esx-1, the best-characterized system, is required for virulence of Mycobacterium tuberculosis, although its precise function during infection remains unclear. Esx-3, a paralogous system present in all mycobacterial species, is required for growth in vitro. Here, we demonstrate that mycobacteria lacking Esx-3 are defective in acquiring iron. To compete for the limited iron available in the host and the environment, these organisms use mycobactin, high-affinity iron-binding molecules. In the absence of Esx-3, mycobacteria synthesize mycobactin but are unable to use the bound iron and are impaired severely for growth during macrophage infection. Mycobacteria thus require a specialized secretion system for acquiring iron from siderophores.

SUBMITTER: Siegrist MS 

PROVIDER: S-EPMC2774023 | biostudies-literature | 2009 Nov

REPOSITORIES: biostudies-literature

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Mycobacterial Esx-3 is required for mycobactin-mediated iron acquisition.

Siegrist M Sloan MS   Unnikrishnan Meera M   McConnell Matthew J MJ   Borowsky Mark M   Cheng Tan-Yun TY   Siddiqi Noman N   Fortune Sarah M SM   Moody D Branch DB   Rubin Eric J EJ  

Proceedings of the National Academy of Sciences of the United States of America 20091021 44


The Esx secretion pathway is conserved across Gram-positive bacteria. Esx-1, the best-characterized system, is required for virulence of Mycobacterium tuberculosis, although its precise function during infection remains unclear. Esx-3, a paralogous system present in all mycobacterial species, is required for growth in vitro. Here, we demonstrate that mycobacteria lacking Esx-3 are defective in acquiring iron. To compete for the limited iron available in the host and the environment, these organi  ...[more]

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