| Literature DB >> 35395239 |
Anna Vlachodimou1, Henk de Vries1, Milena Pasoli1, Miranda Goudswaard1, Soon-Ai Kim2, Yong-Chul Kim2, Mirko Scortichini2, Melissa Marshall3, Joel Linden3, Laura H Heitman4, Kenneth A Jacobson5, Adriaan P IJzerman6.
Abstract
A2B adenosine receptor (A2BAR) antagonists have therapeutic potential in inflammation-related diseases such as asthma, chronic obstructive pulmonary disease and cancer. However, no drug is currently clinically approved, creating a demand for research on novel antagonists. Over the last decade, the study of target binding kinetics, along with affinity and potency, has been proven valuable in early drug discovery stages, as it is associated with improved in vivo drug efficacy and safety. In this study, we report the synthesis and biological evaluation of a series of xanthine derivatives as A2BAR antagonists, including an isothiocyanate derivative designed to bind covalently to the receptor. All 28 final compounds were assessed in radioligand binding experiments, to evaluate their affinity and for those qualifying, kinetic binding parameters. Both structure-affinity and structure-kinetic relationships were derived, providing a clear relationship between affinity and dissociation rate constants. Two structurally similar compounds, 17 and 18, were further evaluated in a label-free assay due to their divergent kinetic profiles. An extended cellular response was associated with long A2BAR residence times. This link between a ligand's A2BAR residence time and its functional effect highlights the importance of binding kinetics as a selection parameter in the early stages of drug discovery.Entities:
Keywords: A(2B) adenosine receptor; Antagonists; Binding kinetics; Covalent binding; Label-free functional assay; Radioligand binding assay
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Year: 2022 PMID: 35395239 PMCID: PMC9358681 DOI: 10.1016/j.bcp.2022.115027
Source DB: PubMed Journal: Biochem Pharmacol ISSN: 0006-2952 Impact factor: 6.100