Abstract
AbstractThe highly trans‐stereoselective reaction of oxyphosphonium enolate (OPE) with N‐benzylidene‐4‐methoxybenzenesulfonamide (N‐BMS) in toluene, at room temperature leading to trans‐aziridine‐2‐carboxylate (trans‐Az 3), was theoretically studied using molecular electron density theory (MEDT) at the B3LYP/6‐31G(d) computational level to shed light on the energy transformation, selectivities, and mechanistic aspects. This domino process is initialized by adding of N,N,N′,N′,N″,N″‐hexamethylphosphanetriamine (HMPT) to methyl benzoylformate to generate OPE. Subsequently, nucleophilic addition of OPE to the C–N double bond in N‐BMS leads to the intermediate IN‐Ta. Finally, trans‐Az 3 is formed through a 3‐exo‐tet ring closure step as a result of the nucleophilic attack of the negatively charged nitrogen atom on the carbon atom bearing –OP (NMe2)3 in IN‐Ta. Analysis of the relative Gibbs free energies shows that the ring closure step is the rate‐determining step. By an investigation of the conceptual density functional theory reactivity indices, OPE and N‐BMS are classified as a strong nucleophilic and as a strong electrophilic species, respectively, which indicates that the additional step of OPE to N‐BMS should display a high‐polar character. An analysis of the calculated electrophilic and nucleophilic Parr functions at the reactive sites of reagents clarifies the regioselectivity observed experimentally along the C1–C2 bond formation process.
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