1. Controlling the Dissociation of Ligands from the Adenosine A2A Receptor through Modulation of Salt Bridge Strength
- Author
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Andrew S. Doré, James C. Errey, Laura H. Heitman, Adriaan P. IJzerman, Fiona H. Marshall, Elena Segala, Francesca Deflorian, Robert M. Cooke, Dong Guo, Robert K. Y. Cheng, and Andrea Bortolato
- Subjects
Models, Molecular ,0301 basic medicine ,Receptor, Adenosine A2A ,Stereochemistry ,Adenosine A2A receptor ,Crystallography, X-Ray ,Ligands ,Protein Engineering ,Dissociation (chemistry) ,Structure-Activity Relationship ,03 medical and health sciences ,Drug Discovery ,Humans ,Receptor ,Cells, Cultured ,G protein-coupled receptor ,Dose-Response Relationship, Drug ,Molecular Structure ,Triazines ,Ligand ,Chemistry ,Drug discovery ,Protein engineering ,Triazoles ,Adenosine receptor ,HEK293 Cells ,030104 developmental biology ,Molecular Medicine - Abstract
Controlling the Dissociation of Ligands from the Adenosine A2A Receptor through Modulation of Salt Bridge StrengthElena Segala, Dong Guo, Robert K. Y. Cheng, Andrea Bortolato, Francesca Deflorian, Andrew S. Doré, James C. Errey, Laura H. Heitman, Adriaan P. IJzerman, Fiona H. Marshall, and Robert M. CookeHeptares Therapeutics Ltd, Biopark Broadwater Road, Welwyn Garden City AL7 3AX, U.K.Division of Medicinal Chemistry, Leiden Academic Centre for Drug Research (LACDR), Leiden University P.O. Box 9502, 2300 RA Leiden, the NetherlandsAbstractThe association and dissociation kinetics of ligands binding to proteins vary considerably, but the mechanisms behind this variability are poorly understood, limiting their utilization for drug discovery. This is particularly so for G protein-coupled receptors (GPCRs) where high resolution structural information is only beginning to emerge. Engineering the human A2A adenosine receptor has allowed structures to be solved in complex with the reference compound ZM241385 and four related ligands at high resolution. Differences between the structures are limited, with the most pronounced being the interaction of each ligand with a salt bridge on the extracellular side of the receptor. Mutagenesis experiments confirm the role of this salt bridge in controlling the dissociation kinetics of the ligands from the receptor, while molecular dynamics simulations demonstrate the ability of ligands to modulate salt bridge stability. These results shed light on a structural determinant of ligand dissociation kinetics and identify a means by which this property may be optimized.
- Published
- 2016
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