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The discovery of benzanilides as c-Met receptor tyrosine kinase inhibitors by a directed screening approach
Authors:Allen Joanne V  Bardelle Catherine  Blades Kevin  Buttar Dave  Chapman Louise  Colclough Nicola  Dossetter Alexander G  Garner Andrew P  Girdwood Alan  Lambert Christine  Leach Andrew G  Law Brian  Major John  Plant Helen  Slater Anthony M
Affiliation:AstraZeneca R&D, Mereside, Alderley Park, Macclesfield, Cheshire SK10 4TG, UK.
Abstract:A directed screen of a relatively small number of compounds, selected for kinase ATP pocket binding potential, yielded a novel series of hit compounds (1). Hit explosion on two binding residues identified compounds 27 and 43 as the best leads for an optimization program having reduced secondary metabolism, as measured by in vitro rat hepatocytes incubation, leading to oral bio-availability. Structure-activity relationships and molecular modeling have suggested a binding mode for the most potent inhibitor 12.
Keywords:c-Met   Kinase   Directed screening   Ligand efficiency   Secondary metabolism   Bio-isosteres   Decisions   Benzanilides
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