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Tunable Amine‐Reactive Electrophiles for Selective Profiling of Lysine

Kuei‐Chien Tang, Jian Cao, Lisa M. Boatner, Linwei Li, Jonathan Farhi, K. N. Houk, Jennifer Spangle, Keriann M. Backus, Monika Raj

2021Angewandte Chemie International Edition37 citationsDOIOpen Access PDF

Abstract

Proteome profiling by activated esters identified >9000 ligandable lysines but they are limited as covalent inhibitors due to poor hydrolytic stability. Here we report our efforts to design and discover a new series of tunable amine-reactive electrophiles (TAREs) for selective and robust labeling of lysine. The major challenges in developing selective probes for lysine are the high nucleophilicity of cysteines and poor hydrolytic stability. Our work circumvents these challenges by a unique design of the TAREs that form stable adducts with lysine and on reaction with cysteine generate another reactive electrophiles for lysine. We highlight that TAREs exhibit substantially high hydrolytic stability as compared to the activated esters and are non-cytotoxic thus have the potential to act as covalent ligands. We applied these alternative TAREs for the intracellular labeling of proteins in different cell lines, and for the selective identification of lysines in the human proteome on a global scale.

Topics & Concepts

ElectrophileLysineAmine gas treatingProfiling (computer programming)ChemistryCombinatorial chemistryComputer scienceOrganic chemistryBiochemistryAmino acidProgramming languageCatalysisChemical Synthesis and AnalysisFluorine in Organic ChemistryClick Chemistry and Applications