Cell & Bioscience (May 2023)

Hinokitiol-iron complex is a ferroptosis inducer to inhibit triple-negative breast tumor growth

  • Hongting Zhao,
  • Meng Zhang,
  • Jinghua Zhang,
  • Zichen Sun,
  • Wenxin Zhang,
  • Weichen Dong,
  • Chen Cheng,
  • Yongzhong Yao,
  • Kuanyu Li

DOI
https://doi.org/10.1186/s13578-023-01044-0
Journal volume & issue
Vol. 13, no. 1
pp. 1 – 15

Abstract

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Abstract Background Ferroptosis is a unique cell death, dependent on iron and phospholipid peroxidation, involved in massive processes of physiopathology. Tremendous attention has been caught in oncology, particularly for those therapy-resistant cancers in the mesenchymal state prone to metastasis due to their exquisite vulnerability to ferroptosis. Therefore, a therapeutical ferroptosis inducer is now underway to be exploited. Results A natural compound, hinokitiol (hino), has been considered to be an iron chelator. We have a novel finding that hino complexed with iron to form Fe(hino)3 can function as a ferroptosis inducer in vitro. The efficiency, compared with the same concentration of iron, increases nearly 1000 folds. Other iron chelators, ferroptosis inhibitors, or antioxidants can inhibit Fe(hino)3-induced ferroptosis. The complex Fe(hino)3 efficacy is further confirmed in orthotopic triple-negative breast cancer (TNBC) tumor models that Fe(hino)3 significantly boosted lipid peroxidation to induce ferroptosis and significantly reduced the sizes of TNBC cell-derived tumors. The drug’s safety was also evaluated, and no detrimental side effects were found with the tested dosage. Conclusions When entering cells, the chelated iron by hinokitiol as a complex Fe(hino)3 is proposed to be redox-active to vigorously promote the production of free radicals via the Fenton reaction. Thus, Fe(hino)3 is a ferroptosis inducer and, therapeutically, exhibits anti-TNBC activity.

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