The ligand-directed (LD) chemistry provides powerful
tools for
site-specific modification of proteins. We utilized a peptide with
an appended methionine (Met) as a ligand; then, the Met thioether
was modified into sulfonium which enabled a proximity induced group
transfer onto protein cysteine in the vicinity upon peptide–target
binding. The sulfonium warhead could be easily constructed with unprotected
peptides, and the transferable group scope was conducted on model
protein PDZ and its ligand peptides. In addition, a living cell labeling
was successfully achieved.