Nature Communications (Oct 2024)

Methionine-SAM metabolism-dependent ubiquinone synthesis is crucial for ROS accumulation in ferroptosis induction

  • Chaoyi Xia,
  • Pinghui Peng,
  • Wenxia Zhang,
  • Xiyue Xing,
  • Xin Jin,
  • Jianlan Du,
  • Wanting Peng,
  • Fengqi Hao,
  • Zhexuan Zhao,
  • Kejian Dong,
  • Miaomiao Tian,
  • Yunpeng Feng,
  • Xueqing Ba,
  • Min Wei,
  • Yang Wang

DOI
https://doi.org/10.1038/s41467-024-53380-5
Journal volume & issue
Vol. 15, no. 1
pp. 1 – 18

Abstract

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Abstract Ferroptosis is a cell death modality in which iron-dependent lipid peroxides accumulate on cell membranes. Cysteine, a limiting substrate for the glutathione system that neutralizes lipid peroxidation and prevents ferroptosis, can be converted by cystine reduction or synthesized from methionine. However, accumulating evidence shows methionine-based cysteine synthesis fails to effectively rescue intracellular cysteine levels upon cystine deprivation and is unable to inhibit ferroptosis. Here, we report that methionine-based cysteine synthesis is tissue-specific. Unexpectedly, we find that rather than inhibiting ferroptosis, methionine in fact plays an essential role during cystine deprivation-induced ferroptosis. Methionine-derived S-adenosylmethionine (SAM) contributes to methylation-dependent ubiquinone synthesis, which leads to lipid peroxides accumulation and subsequent ferroptosis. Moreover, SAM supplementation synergizes with Imidazole Ketone Erastin in a tumor growth suppression mouse model. Inhibiting the enzyme that converts methionine to SAM protects heart tissue from Doxorubicin-induced and ferroptosis-driven cardiomyopathy. This study broadens our understanding about the intersection of amino acid metabolism and ferroptosis regulation, providing insight into the underlying mechanisms and suggesting the methionine-SAM axis is a promising therapeutic strategy to treat ferroptosis-related diseases.