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An Iterative Approach Guides Discovery of the FabI Inhibitor Fabimycin, a Late-Stage Antibiotic Candidate with In Vivo Efficacy against Drug-Resistant Gram-Negative Infections
[Image: see text] Genomic studies and experiments with permeability-deficient strains have revealed a variety of biological targets that can be engaged to kill Gram-negative bacteria. However, the formidable outer membrane and promiscuous efflux pumps of these pathogens prevent many candidate antibi...
Autores principales: | , , , , , , , , , , , , , , , , , , , , , , , , |
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Formato: | Online Artículo Texto |
Lenguaje: | English |
Publicado: |
American Chemical Society
2022
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Acceso en línea: | https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9413440/ https://www.ncbi.nlm.nih.gov/pubmed/36032774 http://dx.doi.org/10.1021/acscentsci.2c00598 |
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author | Parker, Erica N. Cain, Brett N. Hajian, Behnoush Ulrich, Rebecca J. Geddes, Emily J. Barkho, Sulyman Lee, Hyang Yeon Williams, John D. Raynor, Malik Caridha, Diana Zaino, Angela Shekhar, Mrinal Muñoz, Kristen A. Rzasa, Kara M. Temple, Emily R. Hunt, Diana Jin, Xiannu Vuong, Chau Pannone, Kristina Kelly, Aya M. Mulligan, Michael P. Lee, Katie K. Lau, Gee W. Hung, Deborah T. Hergenrother, Paul J. |
author_facet | Parker, Erica N. Cain, Brett N. Hajian, Behnoush Ulrich, Rebecca J. Geddes, Emily J. Barkho, Sulyman Lee, Hyang Yeon Williams, John D. Raynor, Malik Caridha, Diana Zaino, Angela Shekhar, Mrinal Muñoz, Kristen A. Rzasa, Kara M. Temple, Emily R. Hunt, Diana Jin, Xiannu Vuong, Chau Pannone, Kristina Kelly, Aya M. Mulligan, Michael P. Lee, Katie K. Lau, Gee W. Hung, Deborah T. Hergenrother, Paul J. |
author_sort | Parker, Erica N. |
collection | PubMed |
description | [Image: see text] Genomic studies and experiments with permeability-deficient strains have revealed a variety of biological targets that can be engaged to kill Gram-negative bacteria. However, the formidable outer membrane and promiscuous efflux pumps of these pathogens prevent many candidate antibiotics from reaching these targets. One such promising target is the enzyme FabI, which catalyzes the rate-determining step in bacterial fatty acid biosynthesis. Notably, FabI inhibitors have advanced to clinical trials for Staphylococcus aureus infections but not for infections caused by Gram-negative bacteria. Here, we synthesize a suite of FabI inhibitors whose structures fit permeation rules for Gram-negative bacteria and leverage activity against a challenging panel of Gram-negative clinical isolates as a filter for advancement. The compound to emerge, called fabimycin, has impressive activity against >200 clinical isolates of Escherichia coli, Klebsiella pneumoniae, and Acinetobacter baumannii, and does not kill commensal bacteria. X-ray structures of fabimycin in complex with FabI provide molecular insights into the inhibition. Fabimycin demonstrates activity in multiple mouse models of infection caused by Gram-negative bacteria, including a challenging urinary tract infection model. Fabimycin has translational promise, and its discovery provides additional evidence that antibiotics can be systematically modified to accumulate in Gram-negative bacteria and kill these problematic pathogens. |
format | Online Article Text |
id | pubmed-9413440 |
institution | National Center for Biotechnology Information |
language | English |
publishDate | 2022 |
publisher | American Chemical Society |
record_format | MEDLINE/PubMed |
spelling | pubmed-94134402022-08-27 An Iterative Approach Guides Discovery of the FabI Inhibitor Fabimycin, a Late-Stage Antibiotic Candidate with In Vivo Efficacy against Drug-Resistant Gram-Negative Infections Parker, Erica N. Cain, Brett N. Hajian, Behnoush Ulrich, Rebecca J. Geddes, Emily J. Barkho, Sulyman Lee, Hyang Yeon Williams, John D. Raynor, Malik Caridha, Diana Zaino, Angela Shekhar, Mrinal Muñoz, Kristen A. Rzasa, Kara M. Temple, Emily R. Hunt, Diana Jin, Xiannu Vuong, Chau Pannone, Kristina Kelly, Aya M. Mulligan, Michael P. Lee, Katie K. Lau, Gee W. Hung, Deborah T. Hergenrother, Paul J. ACS Cent Sci [Image: see text] Genomic studies and experiments with permeability-deficient strains have revealed a variety of biological targets that can be engaged to kill Gram-negative bacteria. However, the formidable outer membrane and promiscuous efflux pumps of these pathogens prevent many candidate antibiotics from reaching these targets. One such promising target is the enzyme FabI, which catalyzes the rate-determining step in bacterial fatty acid biosynthesis. Notably, FabI inhibitors have advanced to clinical trials for Staphylococcus aureus infections but not for infections caused by Gram-negative bacteria. Here, we synthesize a suite of FabI inhibitors whose structures fit permeation rules for Gram-negative bacteria and leverage activity against a challenging panel of Gram-negative clinical isolates as a filter for advancement. The compound to emerge, called fabimycin, has impressive activity against >200 clinical isolates of Escherichia coli, Klebsiella pneumoniae, and Acinetobacter baumannii, and does not kill commensal bacteria. X-ray structures of fabimycin in complex with FabI provide molecular insights into the inhibition. Fabimycin demonstrates activity in multiple mouse models of infection caused by Gram-negative bacteria, including a challenging urinary tract infection model. Fabimycin has translational promise, and its discovery provides additional evidence that antibiotics can be systematically modified to accumulate in Gram-negative bacteria and kill these problematic pathogens. American Chemical Society 2022-08-10 2022-08-24 /pmc/articles/PMC9413440/ /pubmed/36032774 http://dx.doi.org/10.1021/acscentsci.2c00598 Text en © 2022 The Authors. Published by American Chemical Society https://creativecommons.org/licenses/by/4.0/Permits the broadest form of re-use including for commercial purposes, provided that author attribution and integrity are maintained (https://creativecommons.org/licenses/by/4.0/). |
spellingShingle | Parker, Erica N. Cain, Brett N. Hajian, Behnoush Ulrich, Rebecca J. Geddes, Emily J. Barkho, Sulyman Lee, Hyang Yeon Williams, John D. Raynor, Malik Caridha, Diana Zaino, Angela Shekhar, Mrinal Muñoz, Kristen A. Rzasa, Kara M. Temple, Emily R. Hunt, Diana Jin, Xiannu Vuong, Chau Pannone, Kristina Kelly, Aya M. Mulligan, Michael P. Lee, Katie K. Lau, Gee W. Hung, Deborah T. Hergenrother, Paul J. An Iterative Approach Guides Discovery of the FabI Inhibitor Fabimycin, a Late-Stage Antibiotic Candidate with In Vivo Efficacy against Drug-Resistant Gram-Negative Infections |
title | An Iterative
Approach Guides Discovery of the FabI
Inhibitor Fabimycin, a Late-Stage Antibiotic Candidate with In Vivo Efficacy against Drug-Resistant Gram-Negative Infections |
title_full | An Iterative
Approach Guides Discovery of the FabI
Inhibitor Fabimycin, a Late-Stage Antibiotic Candidate with In Vivo Efficacy against Drug-Resistant Gram-Negative Infections |
title_fullStr | An Iterative
Approach Guides Discovery of the FabI
Inhibitor Fabimycin, a Late-Stage Antibiotic Candidate with In Vivo Efficacy against Drug-Resistant Gram-Negative Infections |
title_full_unstemmed | An Iterative
Approach Guides Discovery of the FabI
Inhibitor Fabimycin, a Late-Stage Antibiotic Candidate with In Vivo Efficacy against Drug-Resistant Gram-Negative Infections |
title_short | An Iterative
Approach Guides Discovery of the FabI
Inhibitor Fabimycin, a Late-Stage Antibiotic Candidate with In Vivo Efficacy against Drug-Resistant Gram-Negative Infections |
title_sort | iterative
approach guides discovery of the fabi
inhibitor fabimycin, a late-stage antibiotic candidate with in vivo efficacy against drug-resistant gram-negative infections |
url | https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9413440/ https://www.ncbi.nlm.nih.gov/pubmed/36032774 http://dx.doi.org/10.1021/acscentsci.2c00598 |
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