Conformational and docking studies of acyl homoserine lactones as a robust method to investigate bioactive conformations |
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| Institution: | 1. V.E. Zuev Institute of Atmospheric Optics, Russian Academy of Sciences, 1, Akademichesky Avenue, 634055 Tomsk, Russian Federation;2. Groupe de Spectrométrie Moléculaire et Atmosphérique, UMR CNRS 6089, Université de Reims, U.F.R. Sciences, B.P. 1039, 51687 Reims Cedex 2, France;3. AILES Beamline, Synchrotron SOLEIL, L''Orme des Merisiers, St-Aubin BP48, F-91192 Gif-sur-Yvette Cedex, France;4. Sorbonne Université, CNRS, MONARIS, UMR 8233, 4 place Jussieu, Paris, France;5. Jet Propulsion Laboratory, California Institute of Technology, 4800 Oak Grove Drive, Pasadena, CA 91109, USA;6. QUAMER laboratory, Tomsk State University, 36 Lenin Avenue, 634050 Tomsk, Russian Federation |
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| Abstract: | A method aiming at investigating possible bioactive conformations of acyl homoserine lactone (AHL) quorum sensing (QS) modulators is established. The method relies on the exhaustive conformational analysis of AHLs by varying torsion angles around the amide group then on the selection of the closest conformation to those known from co-crystallized XRD data of AHL-receptor complexes. These latter are then docked as rigid ligand within the receptor binding site, leading to interactions with binding site residues which are highly consistent as compared with the data arising from XRD studies. The method is first validated using AHLs for which XRD data of their complexes with their cognate receptor are available, then extended to examples for which the binding mode is still unknown.Three compounds were used to validate the method: hexanoyl homoserine lactone (HHL) as an example of autoinducer, 3-oxo-butanoyl homoserine lactone (OBHL), as a representative model of 3-oxo-AHLs, and 4-(4-chlorophenoxy)butanoyl homoserine lactone (CPOBHL) as an example of a QS inhibitor. The conformational analysis of these three compounds to their cognate protein (TraR, SdiA, LasR and CviR) provides the data which enable the next rigid docking step. Further rigid docking of the closest conformations compared to the known bioactive ones within the binding sites allows to recover the expected binding mode with high precision (atomic RMSD < 2 Å). This “conformational analysis/torsion angle filter/rigid ligand docking” method was then used for investigating three non-natural AHL-type QS inhibitors without known co-crystallized XRD structures, namely was 2-hexenoyl homoserine lactone (HenHL), 3-oxo-4-phenylbutanoyl homoserine lactone (OPBHL) and 3-(4-bromophenyl)propanoyl homoserine lactone (BPPHL). Results provide insights into their possible binding mode by identifying specific interactions with some key residues within the receptor binding site, allowing discussion of their biological activity. |
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| Keywords: | Conformational analysis Acyl homoserine lactone Quorum sensing Docking |
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