1. Hydrogenolysis of Carboxylic Ortho Esters
Renat Kadyrov J Org Chem. 2022 Oct 7;87(19):12673-12676. doi: 10.1021/acs.joc.2c01116. Epub 2022 Sep 8.
It is demonstrated for the first time that carboxylic ortho esters may be reduced to acetals using hydrogen as the reducing agent. Hydrogenolysis was performed under mild conditions over commercially available hydrogenation catalysts (5% Pd/C and 5% Pt/C). The present method is especially useful for the selective transformation of carboxylic acids and lactones into acetals.
2. Bioanalysis of plasma acetate levels without derivatization by LC-MS/MS
Rani J Qasem, Ibrahim K Frah, Ahmad S Aljada, Faisal A Sehli Bioanalysis. 2021 Mar;13(5):373-386. doi: 10.4155/bio-2020-0294. Epub 2021 Mar 4.
Background: The acetate ion has important physiological functions and important therapeutic applications. A rapid LC-MS/MS method is described to measure acetate ions in human plasma without chemical derivatization. Materials & methods: A 200 μl sample was spiked with the internal standard 1,2-13C-acetate and proteins precipitated with trichloroacetic acid. The supernatant was recovered and separated under acidic conditions on a C18-column. The eluent was alkalinized by post-column infusion of methanolic ammonium hydroxide. Acetate ions were monitored on a low resolution mass spectrometer in negative ion mode. Results: Method was validated for accuracy and precision with a lower limit of quantitation of 9.7 μM and linear dynamic range up to 339.6 μM. Conclusion: The method is open for analytical improvement and adapts with metabolomic and pharmacometabolomic studies on chemicals of similar nature.
3. Hydride-Abstraction-Initiated Catalytic Stereoselective Intermolecular Bond-Forming Processes
Lei Liu Acc Chem Res. 2022 Dec 6;55(23):3537-3550. doi: 10.1021/acs.accounts.2c00638. Epub 2022 Nov 17.
The stereoselective intermolecular bond-forming reactions through the direct manipulation of ubiquitous yet inert C(sp3)-H bonds represent an important and long-standing goal in chemistry. In particular, developing such a stereoselective bimolecular transformation involving carbocation intermediates generated via site-selective hydride abstraction or formal hydride abstraction by organic oxidants would avoid the preinstallation of directing groups and is therefore attractive. Hydride-abstraction-initiated bimolecular transformations have received considerable attention, but existing examples lack stereoselective studies. Prevalent stereoselective studies typically suffer from the narrow substrate scope of specific and highly reactive N-aryl amines and diarylmethanes together with limited synthetic utility. This Account describes our recent advances in the development and synthetic application of hydride-abstraction-initiated stereoselective intermolecular C-C and C-H bond-forming processes with significantly expanded scopes involving structurally diverse N-acyl amines and ethers together with nitriles, esters, and perfluoroalkyl moieties.We first explored hydride-abstraction-initiated stereoselective intermolecular C-C bond-forming processes. Utilizing triarylmethyl cations or oxoammonium ions as hydride abstractors, we accomplished the diastereoselective oxidative C-H functionalization of structurally diverse N-acyl amines and ethers with a range of organoboranes and C-H components, efficiently installing a series of alkyl, alkenyl, aryl, and alkynyl species into the α-position of heteroatoms with good levels of diastereocontrol. Subsequently, we developed an "acetal pool" strategy as the toolbox to regulate the stability of cationic intermediates and the compatibility of organic oxidants with a delicate asymmetric catalysis system. Utilizing this strategy, we achieved the catalytic enantioselective oxidative C-H alkenylation, arylation, alkynylation, and alkylation of diverse N-acyl heterocycles with a range of boronates and C-H components. Simultaneously, we extended this strategy to the asymmetric oxidative C-H alkylation of ethers. Notably, the method allows solvents that are used daily, such as tetrahydrofuran, tetrahydropyran, and diethyl ether, to be facilely transformed to high-value-added optically pure bioactive molecules. We further expanded the scope of this challenging area from the C(sp3)-H bond adjacent to electron-donating heteroatoms to valuable electron-withdrawing functional groups including nitriles, esters, and perfluoroalkyl moieties for the stereoselective construction of single and vicinal quaternary carbon stereocenters, respectively.We studied hydride-abstraction-initiated catalytic asymmetric intermolecular C-H bond-forming processes, known as redox deracemization. Utilizing the acetal pool strategy, we reported the first redox deracemization of cyclic benzylic ethers. Later, we disclosed an aerobic one-pot deracemization of diverse α-amino acid derivatives with excellent functional group compatibility. We further achieved the deracemization of the tertiary stereogenic center adjacent to electron-withdrawing groups including perfluoroalkyl, cyano, and ester moieties, which are otherwise difficult to construct.
