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Abstract
ATP-competitive kinase inhibitors form hydrogen bond interactions with the kinase hinge region at the adenine binding site. Thus, it is crucial to explore hinge-ligand recognition as part of a rational drug design strategy. Here, harnessing known ligand-bound kinase structures and experimental assay resources, we first create a kinase structure-assay database (KSAD) containing 2915 nanomolar ligand-bound kinase complexes. Then, using the KSAD, we systematically investigate hinge-ligand binding patterns using interaction fingerprints, thereby delineating 15 different hydrogen-bond interaction modes. We believe these results will be valuable for de novo drug design and/or scaffold hopping of kinase-targeted drugs.
Supplementary materials
Title
Table S1-S4
Description
The kinase structure-assay database and the aligned hinge-ligand interaction fingerprints
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