PLoS ONE (Jan 2018)

Vitamin E hydroquinone is an endogenous regulator of ferroptosis via redox control of 15-lipoxygenase.

  • Andrew Hinman,
  • Charles R Holst,
  • Joey C Latham,
  • Joel J Bruegger,
  • Gözde Ulas,
  • Kevin P McCusker,
  • Akiko Amagata,
  • Dana Davis,
  • Kevin G Hoff,
  • Amanda H Kahn-Kirby,
  • Virna Kim,
  • Yuko Kosaka,
  • Edgar Lee,
  • Stephanie A Malone,
  • Janet J Mei,
  • Steve James Richards,
  • Veronica Rivera,
  • Guy Miller,
  • Jeffrey K Trimmer,
  • William D Shrader

DOI
https://doi.org/10.1371/journal.pone.0201369
Journal volume & issue
Vol. 13, no. 8
p. e0201369

Abstract

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Ferroptosis is a form of programmed cell death associated with inflammation, neurodegeneration, and ischemia. Vitamin E (alpha-tocopherol) has been reported to prevent ferroptosis, but the mechanism by which this occurs is controversial. To elucidate the biochemical mechanism of vitamin E activity, we systematically investigated the effects of its major vitamers and metabolites on lipid oxidation and ferroptosis in a striatal cell model. We found that a specific endogenous metabolite of vitamin E, alpha-tocopherol hydroquinone, was a dramatically more potent inhibitor of ferroptosis than its parent compound, and inhibits 15-lipoxygenase via reduction of the enzyme's non-heme iron from its active Fe3+ state to an inactive Fe2+ state. Furthermore, a non-metabolizable isosteric analog of vitamin E which retains antioxidant activity neither inhibited 15-lipoxygenase nor prevented ferroptosis. These results call into question the prevailing model that vitamin E acts predominantly as a non-specific lipophilic antioxidant. We propose that, similar to the other lipophilic vitamins A, D and K, vitamin E is instead a pro-vitamin, with its quinone/hydroquinone metabolites responsible for its anti-ferroptotic cytoprotective activity.