Discovery of Two Highly Selective Structurally Orthogonal Chemical Probes for Activin Receptor-like Kinases 1 and 2\n

Němec, V.; Remeš, M.; Beňovský, P.; Bock, M. C.; Šranková, E.; Fu Wong, J.; Cros, J.; Williams, E.; Hang Tse, L.; Smil, D.; Ensan, D.; Isaac, M. B.; Al-Awar, R.; Gomolková, Regina; Ursachi, V.; Fafílek, Bohumil; Kahounová, Zuzana; Víchová, Ráchel; Vacek, Ondřej; Berger, B.T.; Wells, C. I.; Corona, C. R.; Vasta, J. D.; Roberts, M. B.; Krejčí, Pavel; Souček, Karel; Bullock, A. N.

doi:https://dx.doi.org/10.1021/acs.jmedchem.4c00629

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Discovery of Two Highly Selective Structurally Orthogonal Chemical Probes for Activin Receptor-like Kinases 1 and 2\n

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0602077 - ÚŽFG 2025 RIV US eng J - Journal Article
Němec, V. - Remeš, M. - Beňovský, P. - Bock, M. C. - Šranková, E. - Fu Wong, J. - Cros, J. - Williams, E. - Hang Tse, L. - Smil, D. - Ensan, D. - Isaac, M. B. - Al-Awar, R. - Gomolková, Regina - Ursachi, V. - Fafílek, Bohumil - Kahounová, Zuzana - Víchová, Ráchel - Vacek, Ondřej - Berger, B.T. - Wells, C. I. - Corona, C. R. - Vasta, J. D. - Roberts, M. B. - Krejčí, Pavel - Souček, Karel - Bullock, A. N.
Discovery of Two Highly Selective Structurally Orthogonal Chemical Probes for Activin Receptor-like Kinases 1 and 2
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Journal of Medicinal Chemistry. Roč. 67, č. 15 (2024), s. 12632-12659. ISSN 0022-2623. E-ISSN 1520-4804
R&D Projects: GA MŠMT LM2023052; GA MZd(CZ) NW24-08-00280; GA MŠMT LX22NPO5102
Institutional support: RVO:67985904 ; RVO:68081707
Keywords : activin receptor-like kinases 1 and 2 * protein kinases
OECD category: Biochemistry and molecular biology
Impact factor: 6.9, year: 2023 ; AIS: 1.652, rok: 2023
Method of publishing: Open access
Result website:
https://pubs.acs.org/doi/10.1021/acs.jmedchem.4c00629DOI: https://doi.org/10.1021/acs.jmedchem.4c00629

Activin receptor-like kinases 1-7 (ALK1-7) regulate a complex network of SMAD-independent as well as SMAD-dependent signaling pathways. One of the widely used inhibitors for functional investigations of these processes, in particular for bone morphogenetic protein (BMP) signaling, is LDN-193189. However, LDN-193189 has insufficient kinome-wide selectivity complicating its use in cellular target validation assays. Herein, we report the identification and comprehensive characterization of two chemically distinct highly selective inhibitors of ALK1 and ALK2, M4K2234 and MU1700, along with their negative controls. We show that both MU1700 and M4K2234 efficiently block the BMP pathway via selective in cellulo inhibition of ALK1/2 kinases and exhibit favorable in vivo profiles in mice. MU1700 is highly brain penetrant and shows remarkably high accumulation in the brain. These high-quality orthogonal chemical probes offer the selectivity required to become widely used tools for in vitro and in vivo investigation of BMP signaling.
Permanent Link: https://hdl.handle.net/11104/0359289

Number of the records: 1