4.4 Article

Identification of the Staphylococcus aureus vfrAB Operon, a Novel Virulence Factor Regulatory Locus

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INFECTION AND IMMUNITY
卷 82, 期 5, 页码 1813-1822

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AMER SOC MICROBIOLOGY
DOI: 10.1128/IAI.01655-13

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资金

  1. National Institutes of Health grants [PO1AI83211]
  2. University of New Mexico Infectious Diseases and Inflammation Training [T32-AI007538]
  3. [AH1263]
  4. [AH1458]
  5. [AH1919]
  6. [AI091917]

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During a screen of the Nebraska Transposon Mutant Library, we identified 71 mutations in the Staphylococcus aureus genome that altered hemolysis on blood agar medium. Although many of these mutations disrupted genes known to affect the production of alpha-hemolysin, two of them were associated with an apparent operon, designated vfrAB, that had not been characterized previously. Interestingly, a Delta vfrB mutant exhibited only minor effects on the transcription of the hla gene, encoding alpha-hemolysin, when grown in broth, as well as on RNAIII, a posttranscriptional regulatory RNA important for alpha-hemolysin translation, suggesting that VfrB may function at the posttranscriptional level. Indeed, a Delta vfrB mutant had increased aur and sspAB protease expression under these conditions. However, disruption of the known secreted proteases in the Delta vfrB mutant did not restore hemolytic activity in the Delta vfrB mutant on blood agar. Further analysis revealed that, in contrast to the minor effects of VfrB on hla transcription when strains were cultured in liquid media, the level of hla transcription was decreased 50-fold in the absence of VfrB on solid media. These results demonstrate that while VfrB represses protease expression when strains are grown in broth, hla regulation is highly responsive to factors associated with growth on solid media. Intriguingly, the Delta vfrB mutant displayed increased pathogenesis in a model of S. aureus dermonecrosis, further highlighting the complexity of VfrB-dependent virulence regulation. The results of this study describe a phenotype associated with a class of highly conserved yet un-characterized proteins found in Gram-positive bacteria, and they shed new light on the regulation of virulence factors necessary for S. aureus pathogenesis.

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