iScience (Apr 2024)

Oxidative stress is intrinsic to staphylococcal adaptation to fatty acid synthesis antibiotics

  • Paprapach Wongdontree,
  • Aaron Millan-Oropeza,
  • Jennifer Upfold,
  • Jean-Pierre Lavergne,
  • David Halpern,
  • Clara Lambert,
  • Adeline Page,
  • Gérald Kénanian,
  • Christophe Grangeasse,
  • Céline Henry,
  • Agnès Fouet,
  • Karine Gloux,
  • Jamila Anba-Mondoloni,
  • Alexandra Gruss

Journal volume & issue
Vol. 27, no. 4
p. 109505

Abstract

Read online

Summary: Antibiotics inhibiting the fatty acid synthesis pathway (FASII) of the major pathogen Staphylococcus aureus reach their enzyme targets, but bacteria continue growth by using environmental fatty acids (eFAs) to produce phospholipids. We assessed the consequences and effectors of FASII-antibiotic (anti-FASII) adaptation. Anti-FASII induced lasting expression changes without genomic rearrangements. Several identified regulators affected the timing of adaptation outgrowth. Adaptation resulted in decreased expression of major virulence factors. Conversely, stress responses were globally increased and adapted bacteria were more resistant to peroxide killing. Importantly, pre-exposure to peroxide led to faster anti-FASII-adaptation by stimulating eFA incorporation. This adaptation differs from reports of peroxide-stimulated antibiotic efflux, which leads to tolerance. In vivo, anti-FASII-adapted S. aureus killed the insect host more slowly but continued multiplying. We conclude that staphylococcal adaptation to FASII antibiotics involves reprogramming, which decreases virulence and increases stress resistance. Peroxide, produced by the host to combat infection, favors anti-FASII adaptation.

Keywords