Bis-sulfonamido-2-phenylbenzoxazoles Validate the GroES/EL Chaperone System as a Viable Antibiotic Target

  • Jack Godek
  • , Jared Sivinski
  • , Edmond R. Watson
  • , Felicidad Lebario
  • , Wenli Xu
  • , Mckayla Stevens
  • , Christopher J. Zerio
  • , Andrew J. Ambrose
  • , Xiaoyi Zhu
  • , Carlee A. Trindl
  • , Donna D. Zhang
  • , Steven M. Johnson
  • , Gabriel C. Lander
  • , Eli Chapman

Research output: Contribution to journalArticlepeer-review

5 Scopus citations

Abstract

We recently reported on small-molecule inhibitors of the GroES/GroEL chaperone system as potential antibiotics against Escherichia coli and the ESKAPE pathogens but were unable to establish GroES/GroEL as the cellular target, leading to cell death. In this study, using two of our most potent bis-sulfonamido-2-phenylbenzoxazoles (PBZs), we established the binding site of the PBZ molecules using cryo-EM and found that GroEL was the cellular target responsible for the mode of action. Cryo-EM revealed that PBZ1587 binds at the GroEL ring-ring interface (RRI). A cellular reporter assay confirmed that PBZ1587 engaged GroEL in cells, but cellular rescue experiments showed potential off-target effects. This prompted us to explore a closely related analogue, PBZ1038, which is also bound to the RRI. Biochemical characterization showed potent inhibition of Gram-negative chaperonins but much lower potency of chaperonin from a Gram-positive organism, Enterococcus faecium. A cellular reporter assay showed that PBZ1038 also engaged GroEL in cells and that the cytotoxic phenotype could be rescued by a chromosomal copy of E. faecium GroEL/GroES or by expressing a recalcitrant RRI mutant. These data argue that PBZ1038’s antimicrobial action is exerted through inhibition of GroES/GroEL, validating this chaperone system as an antibiotic target.

Original languageEnglish (US)
Pages (from-to)20845-20856
Number of pages12
JournalJournal of the American Chemical Society
Volume146
Issue number30
DOIs
StatePublished - Jul 31 2024
Externally publishedYes

ASJC Scopus subject areas

  • Catalysis
  • Biochemistry
  • General Chemistry
  • Colloid and Surface Chemistry

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