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Regulatory metabolites of vitamin E and their putative relevance for atherogenesis

Journal

REDOX BIOLOGY
Volume 2, Issue -, Pages 495-503

Publisher

ELSEVIER
DOI: 10.1016/j.redox.2014.02.002

Keywords

alpha-Tocopherol; alpha-Tocopherol long-chain metabolites; alpha-13 '-COOH; Atherosclerosis; Macrophage foam cells

Funding

  1. Forschungskreis der Ernahrungsindustrie (FEI) as part of the Arbeitsgemeinschaft industrieller Forschungsvereinigungen (AiF)
  2. Deutsche Forschungsgemeinschaft (DFG)

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Vitamin E is likely the most important antioxidant in the human diet and alpha-tocopherol is the most active isomer, alpha-Tocopherol exhibits anti-oxidative capacity in vitro, and inhibits oxidation of La. Beside this, alpha-tocopherol shows anti-inflammatory activity and modulates expression of proteins involved in uptake, transport and degradation of tocopherols, as well as the uptake, storage and export of lipids such as cholesterol. Despite promising anti-atherogenic features in vitro, vitamin E failed to be atheroprotective in clinical trials in humans. Recent studies highlight the importance of long-chain metabolites of alpha-tocopherol, which are formed as catabolic intermediate products in the liver and occur in human plasma. These metabolites modulate inflammatory processes and macrophage foam cell formation via mechanisms different than that of their metabolic precursor alpha-tocopherol and at lower concentrations. Here we summarize the controversial role of vitamin E as a preventive agent against atherosclerosis and point the attention to recent findings that highlight a role of these long-chain metabolites of vitamin E as a proposed new class of regulatory metabolites. We speculate that the metabolites contribute to physiological as well as pathophysiological processes. (C) 2014 The Authors. Published by Elsevier B.V.

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