Rhodium carboxylate-mediated reactions of diazoketones involving cyclopropanation, C-H insertion, and aromatic C-C double bond addition/electrocyclic ring opening obey saturation (Michaelis-Menten) kinetics. Axial ligands for rhodium, including aromatic hydrocarbons and Lewis bases such as nitriles, ethers, and ketones, inhibit these reactions by a mixed kinetic inhibition mechanism, meaning that they can bind both to the free catalyst and to the catalyst-substrate complex. Substrate inhibition can also be exhibited by diazocompounds bearing these groupings in addition to the diazo group. The analysis of inhibition shows that the active catalyst uses only one of its two coordination sites at a time for catalysis. Some ketones exhibit the interesting property that they selectively bind to the catalyst-substrate complex. The similarity of the kinetic constants from different types of reactions with similar diazoketones, regardless of the linking unit or the environment of the reacting alkene, suggests that the rate-determining step is the generation of the rhodium carbenoid. A very useful rhodium carboxylate catalyst for asymmetric synthesis, Rh(2)(DOSP)(4), shows slightly slower kinetic parameters than the achiral catalysts, implying that enantioselectivity of this catalyst is based on slowing reactions from one of the enantiotopic faces of the reactant, rather than any type of ligand-accelerated catalysis. A series of rhodium catalysts derived from acids with pK(a)s spanning 4 orders of magnitude give very similar kinetic constants.
Asymmetric rhodium-catalyzed hydroacylation has been utilized in the synthesis of 3-substituted indanones with high conversions and enantioselectivity. The hydroacylation reaction of 2-vinyl benzaldehyde had been previously reported to give a low yield of indanone and an unidentified product. We have identified this compound as a dimer of the starting material. Substitution at the alpha-position of the 2-vinyl benzaldehyde substrates blocks the competitive dimerization reaction and allows the reaction to proceed with yields generally greater than 90%. Utilization of BINAP as a chiral ligand results in good chemical yields and enantioselectivity greater than 95% in most cases.
All-electron numerical density functional theory calculations with scalar relativistic corrections have been utilized to examine the mechanism of the intramolecular rhodium-catalyzed hydroacylation reaction. The gas-phase results reveal a key branch point early in the reaction at the oxidative addition step wherein the two important pathways evolve through five-coordinate Rh(III) intermediates characterized by an apical acyl group and an equatorial hydride, orientations seemingly counter to trans influence arguments. These pathways account for the gross features of the experimental product distribution as well as the isotope labeling outcomes observed by previous investigators in this area. A greatly simplified approximation to modeling the reaction environment was applied that focused on redressing the coordinative unsaturation prevalent during certain steps of the catalytic process by including an explicit molecule of solvent or an additional molecule of substrate. Such an approach allowed us to explain the catalytic deactivation, substrate inhibition and dependence of the reaction rate on this coordinated ligand. Importantly, the application of a popular QM/MM method was unable to locate some of the key stationary points along the reaction path.
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