Xiaoqiang Huang

A reaction design is reported in which a substrate-bound chiral Lewis acid complex absorbs visible light and generates an excited state that directly reacts with a cosubstrate in a highly stereocontrolled fashion. Specifically, a chiral rhodium complex catalyzes visible-light-activated intermolecular [2+2] cycloadditions, providing a wide range of cyclobutanes with up to >99% ee and up to >20:1 d.r. Noteworthy is the ability to create vicinal all-carbon-quaternary stereocenters including spiro centers in an intermolecular fashion.

Aspects of sustainability are playing an increasingly important role for the development of new synthetic methods. In this context, the combination of asymmetric catalysis, which is considered one of the most economic strategies to generate nonracemic chiral compounds, and visible light as an abundant source of energy to induce or activate chemical reactions has recently gained much attention. Furthermore, the combination of photochemistry with asymmetric catalysis provides new opportunity for the development of mechanistically unique reaction schemes. However, the development of such asymmetric photocatalysis is very challenging and two main problems can be pinpointed to undesirable photochemical background reactions and to difficulties in controlling the stereochemistry with photochemically generated highly reactive intermediates. In this Account, we present and discuss asymmetric photocatalysis using one of the currently most versatile photoactivatable asymmetric catalysts, namely, reactive bis-cyclometalated rhodium(III) complexes. The catalysts contain two inert cyclometalating 5-( tert-butyl)-2-phenyl benzoxazole or benzothiazole ligands together with two labile acetonitriles, and the overall chirality is due to a stereogenic metal center. The bis-cyclometalated rhodium complexes serve as excellent chiral Lewis acids for substrates such as 2-acyl imidazoles and N-acyl pyrazoles, which, upon replacement of the two labile acetonitrile ligands, coordinate to the rhodium center in a 2-point fashion. These rhodium-substrate intermediates display unique photophysical and photochemical properties and are often the photoactive intermediates in the developed asymmetric photocatalysis reaction schemes. This combination of visible light excitation to generate long-lived photoexcited states and intrinsic Lewis acid reactivity opens the door for a multitude of visible-light-induced asymmetric conversions. In a first mode of reactivity, bis-cyclometalated rhodium complexes function as chiral Lewis acids to control asymmetric radical reactions of rhodium enolates with electron-deficient radicals, rhodium-coordinated enones with electron-rich radicals, or rhodium-bound radicals generated by photoinduced single electron transfer. The rhodium-substrate complexes in their ground states are key intermediates of the asymmetric catalysis, while separate photoredox cycles initiate radical generations via single electron transfer with either the rhodium-substrate complexes or additional photoactive compounds serving as the photoredox catalyst (secondary asymmetric photocatalysis). In a second mode of reactivity, the rhodium-substrate complexes serve as photoexcited intermediates within the asymmetric catalysis cycle (primary asymmetric photocatalysis) and undergo stereocontrolled chemistry either upon single electron transfer or by direct bond forming reactions out of the excited state. These multiple modes of intertwining photochemistry with asymmetric catalysis have been applied to asymmetric α- and β-alkylations, α- and β-aminations, β-C-H functionalization of carbonyl compounds, [3 + 2] photocycloadditions between cyclopropanes and alkenes or alkynes, [2 + 2] photocycloadditions of enones with alkenes, dearomative [2 + 2] photocycloadditions, and [2 + 3] photocycloadditions of enones with vinyl azides. We anticipate that these reaction schemes of chiral bis-cyclometalated rhodium complexes as (photoactive) chiral Lewis acids will spur the development of new photocatalysts for visible-light-induced asymmetric catalysis.

Harnessing biocatalysts for novel abiological transformations is a longstanding goal of synthetic chemistry. Combining the merits of biocatalysis and photocatalysis allows for selective transformations fueled by visible light and offers many advantages including new reactivity, high enantioselectivity, greener syntheses, and high yields. Photoinduced electron or energy transfer enables synthetic methodologies that complement conventional two electron processes or offer orthogonal pathways for developing new reactions. Enzymes are well suited and can be tuned by directed evolution to exert control over open-shell intermediates, thereby suppressing undesirable reactions and delivering high chemo- and stereoselectivities. Within the past decade, the combination of biocatalysis and photocatalysis was mainly focused on exploiting light-regenerated cofactors to function native enzymatic activity. However, recent developments have demonstrated that the combination can unlock new-to-nature chemistry. Particularly, the discovery and application of new strategies are well poised to expand the applications of photobiocatalysis.In the past five years, our lab has been studying the combinations of photocatalysis and biocatalysis that can be applied to create new synthetic methodologies and solve challenges in synthetic organic chemistry. Our efforts have expanded the strategies for combining external photocatalysts with enzymes through the construction of a synergistic cooperative stereoconvergent reduction system consisting of photosensitized energy transfer and ene-reductase-catalyzed alkene reduction. Additionally, our efforts have also extended the capability of cofactor-dependent photoenzymatic systems to include enantioselective bimolecular radical hydroalkylations of alkenes by irradiating electron donor-acceptor complexes comprised of enzymatic redox active cofactors and unnatural substrates.In this Account, we highlight strategies developed by our group and others for combining biocatalysis and photocatalysis with the aim of introducing non-natural reactivity to enzymes. Presently, strategies applied to achieve this goal include the repurposing of natural photoenzymes, the elucidation of new photoreactivity within cofactor-dependent enzymes, the combination of external photocatalysts with enzymes, and the construction of artificial photoenzymes. By demonstrating the successful applications of these strategies for achieving selective new-to-nature transformations, we hope to spur interest in expanding the scope of photobiocatalytic systems through the use and extension of these strategies and creation of new strategies. Additionally, we hope to elucidate the intuition in synergizing the unique capabilities of biocatalysis and photocatalysis so that photobiocatalysis can be recognized as a potential solution to difficult challenges in synthetic organic chemistry.

The Cu-catalyzed aerobic oxidative esterification of simple ketones via C-C bond cleavage has been developed. Varieties of common ketones, even inactive aryl long-chain alkyl ketones, are selectively converted into esters. The reaction tolerates a wide range of alcohols, including primary and secondary alcohols, chiral alcohols with retention of the configuration, electron-deficient phenols, as well as various natural alcohols. The usage of inexpensive copper catalyst, broad substrate scope, and neutral and open air conditions make this protocol very practical. (18)O labeling experiments reveal that oxygenation occurs during this transformation. Preliminary mechanism studies indicate that two novel pathways are mainly involved in this process.