Reported is the identification of the furo[3,2-b]pyridine core as a novel scaffold for potent and highly selective inhibitors of cdc-like kinases (CLKs) and efficient modulators of the Hedgehog signaling pathway. Initially, a diverse target compound set was prepared by synthetic sequences based on chemoselective metal-mediated couplings, including assembly of the furo[3,2-b]pyridine scaffold by copper-mediated oxidative cyclization. Optimization of the subseries containing 3,5-disubstituted furo[3,2-b]pyridines afforded potent, cell-active, and highly selective inhibitors of CLKs. Profiling of the kinase-inactive subset of 3,5,7-trisubstituted furo[3,2-b]pyridines revealed sub-micromolar modulators of the Hedgehog pathway.

Department of Biology Faculty of Medicine Masaryk University Kamenice 5 Brno 625 00 Czech Republic

Department of Chemistry CZ Openscreen Masaryk University Kamenice 5 Brno 625 00 Czech Republic

Department of Cytokinetics Institute of Biophysics CAS Královopolská 135 Brno 612 65 Czech Republic

Institute for Pharmaceutical Chemistry Structural Genomics Consortium Johann Wolfgang Goethe University Max von Laue Strasse 15 60438 Frankfurt am Main Germany

International Clinical Research Centre St Anne's University Hospital Pekařská 53 Brno 656 91 Czech Republic

Max Planck Institute für Molekulare Physiologie Abteilung Chemische Biologie Otto Hahn Strasse 11 44227 Dortmund Germany

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