A FabG inhibitor targeting an allosteric binding site inhibits several orthologs from Gram-negative ESKAPE pathogens. (15th January 2021)
- Record Type:
- Journal Article
- Title:
- A FabG inhibitor targeting an allosteric binding site inhibits several orthologs from Gram-negative ESKAPE pathogens. (15th January 2021)
- Main Title:
- A FabG inhibitor targeting an allosteric binding site inhibits several orthologs from Gram-negative ESKAPE pathogens
- Authors:
- Vella, Peter
Rudraraju, Reshma Srilakshmi
Lundbäck, Thomas
Axelsson, Hanna
Almqvist, Helena
Vallin, Michaela
Schneider, Gunter
Schnell, Robert - Abstract:
- Graphical abstract: Highlights: FabG from the bacterial fatty acid biosynthesis (FAS-II) system is a potential target for antibiotics. Inhibitors were identified by screening FabG proteins from S. typhimurium and to A. baumannii . The most effective compound inhibits FabG orthologs from several pathogenic bacteria. The structure of the target-inhibitor complex reveals an allosteric binding site. The mechanism of action relays on the distortion of the NADP-binding site, and the decreased protein stability. Abstract: The spread of antibiotic resistance within the ESKAPE group of human pathogenic bacteria poses severe challenges in the treatment of infections and maintenance of safe hospital environments. This motivates efforts to validate novel target proteins within these species that could be pursued as potential targets for antibiotic development. Genetic data suggest that the enzyme FabG, which is part of the bacterial fatty acid biosynthetic system FAS-II, is essential in several ESKAPE pathogens. FabG catalyzes the NADPH dependent reduction of 3-keto-acyl-ACP during fatty acid elongation, thus enabling lipid supply for production and maintenance of the cell envelope. Here we report on small-molecule screening on the FabG enzymes from A. baumannii and S . typhimurium to identify a set of µM inhibitors, with the most potent representative (1 ) demonstrating activity against six FabG-orthologues. A co-crystal structure with FabG from A. baumannii (PDB:6T65) confirmsGraphical abstract: Highlights: FabG from the bacterial fatty acid biosynthesis (FAS-II) system is a potential target for antibiotics. Inhibitors were identified by screening FabG proteins from S. typhimurium and to A. baumannii . The most effective compound inhibits FabG orthologs from several pathogenic bacteria. The structure of the target-inhibitor complex reveals an allosteric binding site. The mechanism of action relays on the distortion of the NADP-binding site, and the decreased protein stability. Abstract: The spread of antibiotic resistance within the ESKAPE group of human pathogenic bacteria poses severe challenges in the treatment of infections and maintenance of safe hospital environments. This motivates efforts to validate novel target proteins within these species that could be pursued as potential targets for antibiotic development. Genetic data suggest that the enzyme FabG, which is part of the bacterial fatty acid biosynthetic system FAS-II, is essential in several ESKAPE pathogens. FabG catalyzes the NADPH dependent reduction of 3-keto-acyl-ACP during fatty acid elongation, thus enabling lipid supply for production and maintenance of the cell envelope. Here we report on small-molecule screening on the FabG enzymes from A. baumannii and S . typhimurium to identify a set of µM inhibitors, with the most potent representative (1 ) demonstrating activity against six FabG-orthologues. A co-crystal structure with FabG from A. baumannii (PDB:6T65) confirms inhibitor binding at an allosteric site located in the subunit interface, as previously demonstrated for other sub-µM inhibitors of FabG from P. aeruginosa . We show that inhibitor binding distorts the oligomerization interface in the FabG tetramer and displaces crucial residues involved in the interaction with the co-substrate NADPH. These observations suggest a conserved allosteric site across the FabG family, which can be potentially targeted for interference with fatty acid biosynthesis in clinically relevant ESKAPE pathogens. … (more)
- Is Part Of:
- Bioorganic & medicinal chemistry. Volume 30(2021)
- Journal:
- Bioorganic & medicinal chemistry
- Issue:
- Volume 30(2021)
- Issue Display:
- Volume 30, Issue 2021 (2021)
- Year:
- 2021
- Volume:
- 30
- Issue:
- 2021
- Issue Sort Value:
- 2021-0030-2021-0000
- Page Start:
- Page End:
- Publication Date:
- 2021-01-15
- Subjects:
- Fatty acid biosynthesis -- FAS II -- FabG -- Allosteric -- Inhibitor -- ESKAPE pathogens
Bioorganic chemistry -- Periodicals
Pharmaceutical chemistry -- Periodicals
Biochemistry -- Periodicals
Chemistry, Clinical -- Periodicals
Chemistry, Organic -- Periodicals
Chimie bio-organique -- Périodiques
Chimie pharmaceutique -- Périodiques
615.19 - Journal URLs:
- http://www.sciencedirect.com/science/journal/09680896 ↗
http://www.elsevier.com/journals ↗ - DOI:
- 10.1016/j.bmc.2020.115898 ↗
- Languages:
- English
- ISSNs:
- 0968-0896
- Deposit Type:
- Legaldeposit
- View Content:
- Available online (eLD content is only available in our Reading Rooms) ↗
- Physical Locations:
- British Library DSC - 2089.325000
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- 15508.xml