| Literature DB >> 33975430 |
Csaba Weber1, Melinda Sipos1, Attila Paczal1, Balazs Balint1, Vilibald Kun1, Nicolas Foloppe2, Pawel Dokurno2, Andrew J Massey2, David Lee Walmsley2, Roderick E Hubbard2, James Murray2, Karen Benwell2, Thomas Edmonds3, Didier Demarles4, Alain Bruno3, Mike Burbridge3, Francisco Cruzalegui3, Andras Kotschy1.
Abstract
The kinase DYRK1A is an attractive target for drug discovery programs due to its implication in multiple diseases. Through a fragment screen, we identified a simple biaryl compound that is bound to the DYRK1A ATP site with very high efficiency, although with limited selectivity. Structure-guided optimization cycles enabled us to convert this fragment hit into potent and selective DYRK1A inhibitors. Exploiting the structural differences in DYRK1A and its close homologue DYRK2, we were able to fine-tune the selectivity of our inhibitors. Our best compounds potently inhibited DYRK1A in the cell culture and in vivo and demonstrated drug-like properties. The inhibition of DYRK1A in vivo translated into dose-dependent tumor growth inhibition in a model of ovarian carcinoma.Entities:
Year: 2021 PMID: 33975430 DOI: 10.1021/acs.jmedchem.1c00023
Source DB: PubMed Journal: J Med Chem ISSN: 0022-2623 Impact factor: 7.446