Although small molecule covalent inhibitors have been widely explored, macromolecular covalent inhibitors are more difficult to design and implement. Here we present a strategy to enable a peptide to bind to its target protein covalently via proximity-enabled bioreactivity, improving its activity of inhibiting the p53–Mdm4 interaction by 10-fold.
C. Hoppmann and L. Wang, Chem. Commun., 2016, 52, 5140 DOI: 10.1039/C6CC01226D
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