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2-Ethynylbenzaldehyde-Based, Lysine-Targeting Irreversible Covalent Inhibitors for Protein Kinases and Nonkinases
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Citations
30
References
2023
Year
Medicinal ChemistryDrug TargetBioorganic ChemistryPharmaceutical ChemistryBiochemistryNatural SciencesMedicineRational Drug DesignProtein KinasesCatalytic LysineAnti-cancer AgentDrug DevelopmentChemical BiologyPharmacologyLysine-targeting StrategyInhibitory ActivityDrug DiscoveryAbl Kinase
Lysine-targeting irreversible covalent inhibitors have attracted growing interests in recent years, especially in the fields of kinase research. Despite encouraging progress, few chemistries are available to develop inhibitors that are exclusively lysine-targeting, selective, and cell-active. We report herein a 2-ethynylbenzaldehyde (EBA)-based, lysine-targeting strategy to generate potent and selective small-molecule inhibitors of ABL kinase by selectively targeting the conserved catalytic lysine in the enzyme. We showed the resulting compounds were cell-active, capable of covalently engaging endogenous ABL kinase in K562 cells with long-residence time and few off-targets. We further validated the generality of this strategy by developing EBA-based irreversible inhibitors against EGFR (a kinase) and Mcl-1 (a nonkinase) that covalently reacted with the catalytic and noncatalytic lysine within each target.
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