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Application of Off-Rate Screening in the Identification of Novel Pan-Isoform Inhibitors of Pyruvate Dehydrogenase Kinase.

Paul A BroughLisa BakerSimon BedfordKirsten BrownSeema ChavdaVictoria ChellJalanie D'AlessandroNicholas G M DaviesBen DavisLoic Le StratAlba T MaciasDaniel MaddoxPatrick C MahonAndrew J MasseyNatalia MatassovaSean McKennaJohannes W G MeissnerJonathan D MooreJames B MurrayChristopher J NorthfieldCharles ParryRachel ParsonsStephen D RoughleyTerry ShawHeather SimmoniteStephen StokesAllan SurgenorEmma StefaniakAlan RobertsonYikang WangPaul WebbNeil WhiteheadMike Wood
Published in: Journal of medicinal chemistry (2017)
Libraries of nonpurified resorcinol amide derivatives were screened by surface plasmon resonance (SPR) to determine the binding dissociation constant (off-rate, kd) for compounds binding to the pyruvate dehydrogenase kinase (PDHK) enzyme. Parallel off-rate measurements against HSP90 and application of structure-based drug design enabled rapid hit to lead progression in a program to identify pan-isoform ATP-competitive inhibitors of PDHK. Lead optimization identified selective sub-100-nM inhibitors of the enzyme which significantly reduced phosphorylation of the E1α subunit in the PC3 cancer cell line in vitro.
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