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

doi:10.1021/jacs.4c05057

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 journal › Article › peer-review

1 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 language	English (US)
Pages (from-to)	20845-20856
Number of pages	12
Journal	Journal of the American Chemical Society
Volume	146
Issue number	30
DOIs	https://doi.org/10.1021/jacs.4c05057
State	Published - Jul 31 2024
Externally published	Yes

ASJC Scopus subject areas

Catalysis
General Chemistry
Biochemistry
Colloid and Surface Chemistry

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Godek, J., Sivinski, J., Watson, E. R., Lebario, F., Xu, W., Stevens, M., Zerio, C. J., Ambrose, A. J., Zhu, X., Trindl, C. A., Zhang, D. D., Johnson, S. M., Lander, G. C., & Chapman, E. (2024). Bis-sulfonamido-2-phenylbenzoxazoles Validate the GroES/EL Chaperone System as a Viable Antibiotic Target. Journal of the American Chemical Society, 146(30), 20845-20856. https://doi.org/10.1021/jacs.4c05057

Godek, J, Sivinski, J, Watson, ER, Lebario, F, Xu, W, Stevens, M, Zerio, CJ, Ambrose, AJ, Zhu, X, Trindl, CA, Zhang, DD, Johnson, SM, Lander, GC & Chapman, E 2024, 'Bis-sulfonamido-2-phenylbenzoxazoles Validate the GroES/EL Chaperone System as a Viable Antibiotic Target', Journal of the American Chemical Society, vol. 146, no. 30, pp. 20845-20856. https://doi.org/10.1021/jacs.4c05057

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

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{\textquoteright}s antimicrobial action is exerted through inhibition of GroES/GroEL, validating this chaperone system as an antibiotic target.",

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

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AU - Godek, Jack

AU - Sivinski, Jared

AU - Watson, Edmond R.

AU - Lebario, Felicidad

AU - Xu, Wenli

AU - Stevens, Mckayla

AU - Zerio, Christopher J.

AU - Ambrose, Andrew J.

AU - Zhu, Xiaoyi

AU - Trindl, Carlee A.

AU - Zhang, Donna D.

AU - Johnson, Steven M.

AU - Lander, Gabriel C.

AU - Chapman, Eli

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AB - 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.

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

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