An Experimental Toolbox for Structure-Based Hit Discovery for P.?aeruginosa FabF,a Promising Target for Antibiotics |
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| Authors: | Ludvik Olai Espeland Dr Charis Georgiou Dr Raphael Klein Hemalatha Bhukya Prof?Dr Bengt Erik Haug Assoc?Prof?Dr Jarl Underhaug Dr Prathama S Mainkar Prof?Dr Ruth Brenk |
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| Affiliation: | 1. Department of Biomedicine, University of Bergen, Jonas Lies Vei 91, 5020 Bergen, Norway;2. Department of Organic Synthesis & Process Chemistry, CSIR-Indian Institute of Chemical Technology, Tarnaka, Hyderabad, 500007 India;3. Department of Chemistry, University of Bergen, Allégaten 41, 5007 Bergen, Norway |
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| Abstract: | FabF (3-oxoacyl-acyl-carrier-protein] synthase 2), which catalyses the rate limiting condensation reaction in the fatty acid synthesis II pathway, is an attractive target for new antibiotics. Here, we focus on FabF from P. aeruginosa (PaFabF) as antibiotics against this pathogen are urgently needed. To facilitate exploration of this target we have set up an experimental toolbox consisting of binding assays using bio-layer interferometry (BLI) as well as saturation transfer difference (STD) and WaterLOGSY NMR in addition to robust conditions for structure determination. The suitability of the toolbox to support structure-based design of FabF inhibitors was demonstrated through the validation of hits obtained from virtual screening. Screening a library of almost 5 million compounds resulted in 6 compounds for which binding into the malonyl-binding site of FabF was shown. For one of the hits, the crystal structure in complex with PaFabF was determined. Based on the obtained binding mode, analogues were designed and synthesised, but affinity could not be improved. This work has laid the foundation for structure-based exploration of PaFabF. |
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| Keywords: | antibiotics bio-layer interferometry ligand-based NMR structure-based design virtual screening |
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