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

Václav Němec; Prashant Khirsariya; Pavlína Janovská; Paula Martín Moyano; Lukáš Maier; Petra Procházková; Pavlína Kebková; Tomáš Gybel'; Benedict Tilman Berger; Apirat Chaikuad; Maria Reinecke; Bernhard Kuster; Stefan Knapp; Vítězslav Bryja; Kamil Paruch

doi:10.1002/anie.202217532

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

Václav Němec, Prashant Khirsariya, Pavlína Janovská, Paula Martín Moyano, Lukáš Maier, Petra Procházková, Pavlína Kebková, Tomáš Gybel', Benedict Tilman Berger, Apirat Chaikuad, Maria Reinecke, Bernhard Kuster, Stefan Knapp, Vítězslav Bryja, Kamil Paruch

Lehrstuhl für Proteomik und Bioanalytik

Publikation: Beitrag in Fachzeitschrift › Artikel › Begutachtung

6 Zitate (Scopus)

Abstract

Casein 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.

Originalsprache	Englisch
Aufsatznummer	e202217532
Fachzeitschrift	Angewandte Chemie International Edition in English
Jahrgang	62
Ausgabenummer	11
DOIs	https://doi.org/10.1002/anie.202217532
Publikationsstatus	Veröffentlicht - 6 März 2023

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10.1002/anie.202217532

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Němec, V., Khirsariya, P., Janovská, P., Moyano, P. M., Maier, L., Procházková, P., Kebková, P., Gybel', T., Berger, B. T., Chaikuad, A., Reinecke, M., Kuster, B., Knapp, S., Bryja, V., & Paruch, K. (2023). Discovery of Potent and Exquisitely Selective Inhibitors of Kinase CK1 with Tunable Isoform Selectivity. Angewandte Chemie International Edition in English, 62(11), Artikel e202217532. https://doi.org/10.1002/anie.202217532

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title = "Discovery of Potent and Exquisitely Selective Inhibitors of Kinase CK1 with Tunable Isoform Selectivity",

abstract = "Casein 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.",

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doi = "10.1002/anie.202217532",

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Němec, V, Khirsariya, P, Janovská, P, Moyano, PM, Maier, L, Procházková, P, Kebková, P, Gybel', T, Berger, BT, Chaikuad, A, Reinecke, M, Kuster, B, Knapp, S, Bryja, V & Paruch, K 2023, 'Discovery of Potent and Exquisitely Selective Inhibitors of Kinase CK1 with Tunable Isoform Selectivity', Angewandte Chemie International Edition in English, Jg. 62, Nr. 11, e202217532. https://doi.org/10.1002/anie.202217532

TY - JOUR

T1 - Discovery of Potent and Exquisitely Selective Inhibitors of Kinase CK1 with Tunable Isoform Selectivity

AU - Němec, Václav

AU - Khirsariya, Prashant

AU - Janovská, Pavlína

AU - Moyano, Paula Martín

AU - Maier, Lukáš

AU - Procházková, Petra

AU - Kebková, Pavlína

AU - Gybel', Tomáš

AU - Berger, Benedict Tilman

AU - Chaikuad, Apirat

AU - Reinecke, Maria

AU - Kuster, Bernhard

AU - Knapp, Stefan

AU - Bryja, Vítězslav

AU - Paruch, Kamil

PY - 2023/3/6

Y1 - 2023/3/6

N2 - Casein 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.

AB - Casein 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.

KW - CK1

KW - Chemical Probe

KW - Inhibitor

KW - Isoform Selectivity

KW - Wnt Pathway

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U2 - 10.1002/anie.202217532

DO - 10.1002/anie.202217532

M3 - Article

AN - SCOPUS:85147185160

SN - 1433-7851

VL - 62

JO - Angewandte Chemie International Edition in English

JF - Angewandte Chemie International Edition in English

IS - 11

M1 - e202217532

ER -

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

Abstract

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