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Selective Halogenation of Pyridines Using Designed Phosphine Reagents.

Jeffrey N LevyJuan V Alegre-RequenaRenrong LiuRobert S PatonAndrew McNally
Published in: Journal of the American Chemical Society (2020)
Halopyridines are key building blocks for synthesizing pharmaceuticals, agrochemicals, and ligands for metal complexes, but strategies to selectively halogenate pyridine C-H precursors are lacking. We designed a set of heterocyclic phosphines that are installed at the 4-position of pyridines as phosphonium salts and then displaced with halide nucleophiles. A broad range of unactivated pyridines can be halogenated, and the method is viable for late-stage halogenation of complex pharmaceuticals. Computational studies indicate that C-halogen bond formation occurs via an SNAr pathway, and phosphine elimination is the rate-determining step. Steric interactions during C-P bond cleavage account for differences in reactivity between 2- and 3-substituted pyridines.
Keyphrases
  • ionic liquid
  • molecular docking
  • dna binding