Solvent-Switchable Remote C–H Activation via 1,4-Palladium Migration Enables Site-Selective C–P Bond Formation: A Tool for the Synthesis of P‑Chiral Phosphinyl Imidazoles

Solvent-switchable and site-selective phosphorylation of imidazoles at the C2 or C5 position of the imidazole ring was achieved via 1,4-palladium migration. P-Chiral tert-butyl­(aryl)­phosphine oxides were cross-coupled to 1-(2-bromophenyl)-1H-imidazoles with high enantiospecificity, thereby leading to a novel class of chiral imidazole-based phosphine oxides. As proof of concept, reduction of an analogue yielded the corresponding P-chiral 2-phosphinyl imidazole ligand, which was shown to induce high enantioselectivity in the formation of axially chiral molecules synthesized via Pd-catalyzed Suzuki–Miyaura cross-coupling.