Metal-Catalyzed Directed Regio- and Enantioselective Ring-Opening of Epoxides.

Abstract

Control of regio- and stereoselectivity of chemical reactions is the central theme in synthetic chemistry. Regioselective and enantiospecific ring opening of readily available enantioenriched epoxides precursors provides a straightforward access to diverse highly functionalized molecules which can serve as chiral building blocks for synthesis of biologically active compounds. However, prior to our research work, the scope of catalytic highly regioselective ring opening of epoxides is limited to structurally or electronically biased epoxides, such as terminal and aromatic epoxides. Regioselective ring-opening of epoxides with substituents on both sides demonstrating similar steric and electronic effects is still a formidable challenge for organic chemists. To address this challenge, our approach is to use the readily available functional moiety incorporated in an epoxide as a directing group to realize the regioselective nucleophilic attack on the oxirane ring. Alternatively, asymmetric ring-opening of epoxides can also provide the ring-opening products in highly enantioenriched form. However, excellent results are usually obtained in the case of the kinetic resolution of terminal epoxides or the desymmetrization of meso-epoxides. In these cases, the issue of regiocontrol of the ring-opening is circumvented or minimized. Based on our successful results of regioselective ring-opening of functionalized epoxides by implementing the directed ring-opening strategy, we also investigated the enantioselective ring-opening of internal epoxides bearing a functional moiety as directing group. This Account summarizes our research on metal-catalyzed directed ring-opening reactions of epoxides, which encompasses the following breakthroughs: (1) highly regioselective ring-opening of various substrates including epoxy allylic alcohols, epoxy homoallylic alcohols and epoxy allylic sulfonamides with a variety of N-, O-, and halide-nucleophiles catalyzed by W-, Mo-, or Ni-salt; (2) first kinetic resolutions of epoxy allylic alcohols, epoxy homoallylic alcohols, and epoxy allylic sulfonamides with various amines as nucleophiles, which were catalyzed by W-bishydroxamic acid (W-BHA), nickel-BINAM, and Gd-N,N'-dioxide catalytic system, respectively; (3) successful implementation of the strategy of combined asymmetric syntheses by the combination of the enantioselective epoxidation and the enantioselective ring-opening of 2,3-epoxy alcohols establishing a new entry to prepare amino alcohols in regio-, diastereo-, and enantiomerically pure form.