16698-35-4Relevant articles and documents
Kinetics of the reaction by which natural vitamin E is regenerated by vitamin C
Nagaoka, Shin-ichi,Kakiuchi, Takuhiro,Ohara, Keishi,Mukai, Kazuo
, p. 26 - 32 (2007)
The rate constant and activation energy of the regeneration reaction of natural vitamin E by vitamin C were determined with a double-mixing stopped-flow spectrophotometer. The formation of vitamin C radical was observed in the absorption spectrum. The kinetic effect of methyl substitution on the aromatic ring of vitamin E radical indicates that partial charge-transfer plays a role in the reaction. Since a substantial deuterium kinetic isotope effect was not found, the tunneling effect may not play an important role under the present experimental conditions.
Process of separating chiral isomers of chroman compounds and their derivatives and precursors
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Page/Page column 15, (2012/12/13)
The present invention relates to a process of separating chiral isomers of chroman compounds, particularly tocopherols and tocotrienols as well as the esters and intermediates thereof. It has been found that this process allows a separation of the desired isomer with a higher yield and enables the use of the non-desired isomers in a very efficient way. Said process is particularly useful when implemented in an industrial process. Furthermore, it has been found that this process allows using isomer mixtures as they result from traditional industrial synthesis.
Vitamin E chemistry. Nitration of non-α-tocopherols: Products and mechanistic considerations
Patel, Anjan,Liebner, Falk,Netscher, Thomas,Mereiter, Kurt,Rosenau, Thomas
, p. 6504 - 6512 (2008/02/10)
(Chemical Equation Presented) In contrast to the α-form permethylated at the aromatic ring, non-α-tocopherols possess free aromatic ring positions which enable them to act as potent scavengers of electrophiles in vivo and in vitro. In preparation of enzymatic studies involving peroxynitrite and other nitrating systems, the behavior of non-α-tocopherols under nitration conditions was studied. The nitration products of β-, γ-, and δ-tocopherol were identified, comprehensively analytically characterized, and their structure was supported by X-ray crystal structure analysis on truncated model compounds. Even under more drastic nitration conditions, no erosion of the stereochemistry at 2-C occurred. The nitrosation of γ-tocopherol and δ-tocopherol was re-examined, showing the slow oxidation of the initial nitroso products to the corresponding nitro derivatives by air to be superimposed by a fast equilibrium with the tautomeric ortho-quinone monoxime, which only in the case of γ-tocopherol released hydroxyl amine at elevated temperatures to afford the stable ortho-quinone. Mononitration of δ-tocopherol selectively proceeded at position 5. This selectivity can be explained by the theory of strain-induced bond localization (SIBL) to the quinoid nitration intermediates. Bisnitration was only insignificantly disfavored by the first nitro group, so that under normal nitration conditions offering an excess of nitrating species only the bisnitration product was found.
