Affiliation:
1. Department of Chemistry Tianjin Key Laboratory of Molecular Optoelectronic Sciences Frontiers Science Center for Synthetic Biology (Ministry of Education) Tianjin University Tianjin 300072 P. R. China
2. Joint School of National University of Singapore and Tianjin University International Campus of Tianjin University Binhai New City, Fuzhou 350207 P. R. China
Abstract
AbstractCatalytic asymmetric hydrogenation of enamido phosphorus derivatives is one of the most efficient methods for the construction of chiral amino phosphorus products, among which the congested tetra‐substituted substrates remains an unaddressed challenge. In this study, we utilize a commercially available Rh‐Josiphos system for the efficient and stereoselective hydrogenation of a wide set of tetra‐substituted cyclic β‐enamido phosphonates/phosphine oxides, thus enabling access to chiral β‐amino phosphorus compounds featuring two vicinal stereocenters. This protocol was broadly applicable to different ring systems possessing various phosphonate/phosphine oxide groups and further applied in the preparation of amino‐phosphine ligands. DFT mechanistic explorations indicate that the C=C migratory insertion into RhIII−H bond could be the rate‐ and stereo‐determining step. The origins of stereoselectivity are revealed through distortion/interaction analysis, which is primarily regulated by distinguished dispersion interactions and steric repulsions.
Funder
National Natural Science Foundation of China
National Key Research and Development Program of China