4.8 Article

Small-molecule targeting of a diapophytoene desaturase inhibits S. aureus virulence

Journal

NATURE CHEMICAL BIOLOGY
Volume 12, Issue 3, Pages 174-179

Publisher

NATURE PUBLISHING GROUP
DOI: 10.1038/NCHEMBIO.2003

Keywords

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Funding

  1. National Natural Science Foundation of China [21472207, 31270126, 21222211, 91313303]
  2. Hundred Talents Program of the Chinese Academy of Sciences
  3. Shanghai Institute of Materia Medica Foundation [CASIMM0120152018]
  4. Shanghai Municipal Education Commission and Shanghai Education Development Foundation [14SG28]
  5. Foundation of the State Key Laboratory of Drug Research [SIMM1302KF-01]
  6. National Science and Technology Major Project Key New Drug Creation and Manufacturing Program [2013ZX09507-004]

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The surge of antibiotic resistance in Staphylococcus aureus has created a dire need for innovative anti-infective agents that attack new targets, to overcome resistance. In S. aureus, carotenoid pigment is an important virulence factor because it shields the bacterium from host oxidant killing. Here we show that naftifine, a US Food and Drug Administration (FDA)-approved anti fungal drug, blocks biosynthesis of carotenoid pigment at nanomolar concentrations. This effect is mediated by competitive inhibition of S. aureus diapophytoene desaturase (CrtN), an essential enzyme for carotenoid pigment synthesis. We found that naftifine attenuated the virulence of a variety of clinical S. aureus isolates, including methicillin-resistant S. aureus (MRSA) strains, in mouse infection models. Specifically, we determined that naftifine is a lead compound for potent CrtN inhibitors. In sum, these findings reveal that naftifine could serve as a chemical probe to manipulate CrtN activity, providing proof of concept that CrtN is a druggable target against S. aureus infections.

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