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Structure-Guided Modification of Heterocyclic Antagonists of the P2Y14 Receptor.


ABSTRACT: The P2Y14 receptor (P2Y14R) mediates inflammatory activity by activating neutrophil motility, but few classes of antagonists are known. We have explored the structure-activity relationship of a 3-(4-phenyl-1 H-1,2,3-triazol-1-yl)-5-(aryl)benzoic acid antagonist scaffold, assisted by docking and molecular dynamics (MD) simulation at a P2Y14R homology model. A computational pipeline using the High Throughput MD Python environment guided the analogue design. Selection of candidates was based upon ligand-protein shape and complementarity and the persistence of ligand-protein interactions over time. Predictions of a favorable substitution of a 5-phenyl group with thiophene and an insertion of a three-methylene spacer between the 5-aromatic and alkyl amino moieties were largely consistent with empirical results. The substitution of a key carboxylate group on the core phenyl ring with tetrazole or truncation of the 5-aryl group reduced affinity. The most potent antagonists, using a fluorescent assay, were a primary 3-aminopropyl congener 20 (MRS4458) and phenyl p-carboxamide 30 (MRS4478).

SUBMITTER: Yu J 

PROVIDER: S-EPMC6428052 | biostudies-literature | 2018 Jun

REPOSITORIES: biostudies-literature

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Structure-Guided Modification of Heterocyclic Antagonists of the P2Y<sub>14</sub> Receptor.

Yu Jinha J   Ciancetta Antonella A   Dudas Steven S   Duca Sierra S   Lottermoser Justine J   Jacobson Kenneth A KA  

Journal of medicinal chemistry 20180516 11


The P2Y<sub>14</sub> receptor (P2Y<sub>14</sub>R) mediates inflammatory activity by activating neutrophil motility, but few classes of antagonists are known. We have explored the structure-activity relationship of a 3-(4-phenyl-1 H-1,2,3-triazol-1-yl)-5-(aryl)benzoic acid antagonist scaffold, assisted by docking and molecular dynamics (MD) simulation at a P2Y<sub>14</sub>R homology model. A computational pipeline using the High Throughput MD Python environment guided the analogue design. Selecti  ...[more]

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