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An Alkynylpyrimidine-Based Covalent Inhibitor That Targets a Unique Cysteine in NF-κB-Inducing Kinase

Authors :
Lan Z. Wang
Miller Duncan Charles
Bernard T. Golding
Ian Hickson
Martin E.M. Noble
Celine Cano
Suzannah J. Harnor
Michael J. Waring
Harry J Shrives
Shaimaa Khalifa
Jane Totobenazara
Stephen J. Hobson
Elaine Willmore
Hannah L Stewart
Mathew P. Martin
Susan J. Tudhope
Huw D. Thomas
Islam Al-Khawaldeh
Claire E. Jennings
João V de Souza
Max J. Temple
Jane A. Endicott
Cinzia Bordoni
Honorine Lebraud
Agnieszka K. Bronowska
Ian R. Hardcastle
Amy B. Heptinstall
Stephen R. Wedge
Christine Basmadjian
Gregory G Aldred
Julie A. Tucker
Mohammed J Al Yasiri
Source :
Journal of Medicinal Chemistry. 64:10001-10018
Publication Year :
2021
Publisher :
American Chemical Society (ACS), 2021.

Abstract

NF-κB-inducing kinase (NIK) is a key enzyme in the noncanonical NF-κB pathway, of interest in the treatment of a variety of diseases including cancer. Validation of NIK as a drug target requires potent and selective inhibitors. The protein contains a cysteine residue at position 444 in the back pocket of the active site, unique within the kinome. Analysis of existing inhibitor scaffolds and early structure-activity relationships (SARs) led to the design of C444-targeting covalent inhibitors based on alkynyl heterocycle warheads. Mass spectrometry provided proof of the covalent mechanism, and the SAR was rationalized by computational modeling. Profiling of more potent analogues in tumor cell lines with constitutively activated NIK signaling induced a weak antiproliferative effect, suggesting that kinase inhibition may have limited impact on cancer cell growth. This study shows that alkynyl heterocycles are potential cysteine traps, which may be employed where common Michael acceptors, such as acrylamides, are not tolerated.

Details

ISSN :
15204804 and 00222623
Volume :
64
Database :
OpenAIRE
Journal :
Journal of Medicinal Chemistry
Accession number :
edsair.doi.dedup.....56300566066f33b5e78d20a96b537040