4.8 Article

The C terminus of the mycobacterium ESX-1 secretion system substrate ESAT-6 is required for phagosomal membrane damage and virulence

PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA (2022)

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Journal

PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA
Volume 119, Issue 11, Pages -

Publisher

NATL ACAD SCIENCES
DOI: 10.1073/pnas.2122161119

Keywords

ESAT-6; ESX-1; phagosomal damage; virulence

Categories

Multidisciplinary Sciences

Funding

  1. Wellcome Trust Principal Research Fellowship [223103/Z/21/Z]
  2. NIH MERIT award [R37 AI054503]
  3. Wellcome Trust [223103/Z/21/Z] Funding Source: Wellcome Trust

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This study reveals the causal relationship between ESAT-6 membranolysis and ESX-1-mediated virulence in Mycobacterium tuberculosis and Mycobacterium marinum. Mutations in ESAT-6's C-terminal tail residues disrupt phagosomal damage and granuloma formation, while still retaining the ability to lyse acidified liposomes.
Mycobacterium tuberculosis and its close relative Mycobacterium marinum infect macrophages and induce the formation of granulo-mas, organized macrophage-rich immune aggregates. These myco-bacterial pathogens can accelerate and co-opt granuloma formation for their benefit, using the specialized secretion system ESX-1, a key virulence determinant. ESX-1-mediated virulence is attributed to the damage it causes to the membranes of macrophage phagoso-mal compartments, within which the bacteria reside. This phagoso-mal damage, in turn, has been attributed to the membranolytic activity of ESAT-6, the major secreted substrate of ESX-1. However, mutations that perturb ESAT-6's membranolytic activity often result in global impairment of ESX-1 secretion. This has precluded an understanding of the causal and mechanistic relationships between ESAT-6 membranolysis and ESX-1-mediated virulence. Here, we identify two conserved residues in the unstructured C-terminal tail of ESAT-6 required for phagosomal damage, granuloma formation, and virulence. Importantly, these ESAT-6 mutants have near-normal levels of secretion, far higher than the minimal threshold we estab-lish is needed for ESX-1-mediated virulence early in infection. Unex-pectedly, these loss-of-function ESAT-6 mutants retain the ability to lyse acidified liposomes. Thus, ESAT-6's virulence functions in vivo can be uncoupled from this in vitro surrogate assay. These uncou-pling mutants highlight an enigmatic functional domain of ESAT-6 and provide key tools to investigate the mechanism of phagosomal damage and virulence.

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