Transition Metal-Catalyzed Biaryl Atropisomer Synthesis via a Torsional Strain Promoted Ring-Opening Reaction

Abstract

Arising from the restricted rotation of a single bond caused by steric or electronic effects, atropisomerism is one of the few fundamental categories for molecules to manifest their three-dimensional characters into which axially chiral biaryl compounds fall. Despite the widespread occurrence of axially chiral skeletons in natural products, bioactive molecules, and chiral ligands/organocatalysts, catalytic asymmetric methods for the synthesis of these structures still lag behind demand. Major challenges for the preparation of these chiral biaryls include accessing highly sterically hindered variants while controlling the stereoselectivity. A couple of useful strategies have emerged for the direct asymmetric synthesis of these molecules in the last two decades.

Recently, we have engaged in catalytic asymmetric synthesis of biaryl atropisomers via transition metal catalysis, including asymmetric ring-openings of dibenzo cyclic compounds. During these studies, we serendipitously discovered that the two substituents adjacent to the axis cause these dibenzo cyclic molecules to be distorted to minimize steric repulsion. The distorted compounds display higher reactivity in the ring-opening reactions than the non-distorted molecules. In other words, torsional strain can promote a ring-opening reaction. On the basis of this concept, we have successfully realized the catalytic asymmetric ring-opening reaction of cyclic diaryliodoniums, dibenzo silanes, and 9H-fluoren-9-ols, which delivered several differently substituted ortho tetra-substituted biaryl atropisomers in high enantioselectivity. The torsional strain not only activates the substrates toward ring-opening under mild conditions but also changes the chemoselectivity of bond-breaking events. In the palladium-catalyzed carboxylation of S-aryl dibenzothiophenium, the torsional strain inversed the bond selectivity from exocyclic C–S bond cleavage to the ring-opening reaction.

In this Account, we summarize our studies on copper-, rhodium-, or palladium-catalyzed asymmetric ring-opening reactions of dibenzo cyclic compounds as a useful collection of methods for the straightforward preparation of orthotetra-substituted biaryl atropisomers with high enantiopurity on the basis of the above-mentioned torsional strain-promoted ring-opening coupling strategy. In the last part, the torsional strain energies are also discussed with the aid of density functional theory (DFT) calculations.