Discovery of Potent and Exquisitely Selective Inhibitors of Kinase CK1 with Tunable Isoform Selectivity-Reference-Cited by-同舟云学术

Discovery of Potent and Exquisitely Selective Inhibitors of Kinase CK1 with Tunable Isoform Selectivity

Published:2023-02-02 Issue:11 Volume:62 Page:
ISSN:1433-7851
Container-title:Angewandte Chemie International Edition
language:en
Short-container-title:Angew Chem Int Ed

Author:

Němec Václav¹²,Khirsariya Prashant¹²^ORCID,Janovská Pavlína³,Moyano Paula Martín¹,Maier Lukáš¹²,Procházková Petra³,Kebková Pavlína³,Gybel' Tomáš³,Berger Benedict‐Tilman⁴,Chaikuad Apirat⁴,Reinecke Maria⁵,Kuster Bernhard⁵⁶,Knapp Stefan⁴,Bryja Vítězslav³^ORCID,Paruch Kamil¹²^ORCID

Affiliation:

1. Department of Chemistry, Faculty of Science Masaryk University Kamenice 5 Brno 625 00 Czech Republic

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

3. Department of Experimental Biology, Faculty of Science Masaryk University Kamenice 5 Brno 625 00 Czech Republic

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

5. Chair of Proteomics and Bioanalytics TUM School of Life Sciences Technical University of Munich 85354 Freising Germany

6. Bavarian Center for Biomolecular Mass Spectrometry (BayBioMS) Technical University of Munich 85354 Freising Germany

Abstract

AbstractCasein kinases 1 (CK1) are key signaling molecules that have emerged recently as attractive therapeutic targets in particular for the treatment of hematological malignancies. Herein, we report the identification of a new class of potent and highly selective inhibitors of CK1α, δ and ϵ. Based on their optimal in vitro and in vivo profiles and their exclusive selectivity, MU1250, MU1500 and MU1742 were selected as quality chemical probes for those CK1 isoforms. At proper concentrations, MU1250 and MU1500 allow for specific targeting of CK1δ or dual inhibition of CK1δ/ϵ in cells. The compound MU1742 also efficiently inhibits CK1α and, to our knowledge, represents the first potent and highly selective inhibitor of this enzyme. In addition, we demonstrate that the central 1H‐pyrrolo[2,3‐b]pyridine‐imidazole pharmacophore can be used as the basis of highly selective inhibitors of other therapeutically relevant protein kinases, e.g. p38α, as exemplified by the compound MU1299.

Funder

Ministerstvo Školství, Mládeže a Tělovýchovy

Bader Philanthropies

Publisher

Wiley

Subject

General Chemistry,Catalysis

Link

https://onlinelibrary.wiley.com/doi/pdf/10.1002/anie.202217532

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