| Literature DB >> 30362749 |
Victoria Georgi1,2, Felix Schiele1, Benedict-Tilman Berger1,2,3, Andreas Steffen1, Paula A Marin Zapata1, Hans Briem1, Stephan Menz1, Cornelia Preusse1, James D Vasta4, Matthew B Robers4, Michael Brands1, Stefan Knapp2,3, Amaury Fernández-Montalván1.
Abstract
Target residence time is emerging as an important optimization parameter in drug discovery, yet target and off-target engagement dynamics have not been clearly linked to the clinical performance of drugs. Here we developed high-throughput binding kinetics assays to characterize the interactions of 270 protein kinase inhibitors with 40 clinically relevant targets. Analysis of the results revealed that on-rates are better correlated with affinity than off-rates and that the fraction of slowly dissociating drug-target complexes increases from early/preclinical to late stage and FDA-approved compounds, suggesting distinct contributions by each parameter to clinical success. Combining binding parameters with PK/ADME properties, we illustrate in silico and in cells how kinetic selectivity could be exploited as an optimization strategy. Furthermore, using bio- and chemoinformatics we uncovered structural features influencing rate constants. Our results underscore the value of binding kinetics information in rational drug design and provide a resource for future studies on this subject.Mesh:
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Year: 2018 PMID: 30362749 DOI: 10.1021/jacs.8b08048
Source DB: PubMed Journal: J Am Chem Soc ISSN: 0002-7863 Impact factor: 15.419