Nature Communications (Mar 2025)

Quasi Fe MIL-53 nanozyme inducing ferroptosis and immunogenic cell death for cancer immunotherapy

  • Zihui Yan,
  • Yang Bai,
  • Songtao Zhang,
  • Lingyi Kong,
  • Yu Wang,
  • Huilin Sun,
  • Yi Li,
  • Lin Qiu,
  • Ruijie Zhang,
  • Pengju Jiang,
  • Donghui Zhao,
  • Zhongyan Chen,
  • Yafei Li,
  • Huan Pang,
  • Jianhao Wang

DOI
https://doi.org/10.1038/s41467-025-57542-x
Journal volume & issue
Vol. 16, no. 1
pp. 1 – 19

Abstract

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Abstract Nanozymes offer diverse therapeutic potentials for cancer treatment which is dependent on the development of nanomaterials. Quasi-metal-organic framework is a class of metal-organic framework-derived nanomaterials with a transition state from metal-organic frameworks towards metal oxide featuring porous structure and high activity. Herein an iron-based quasi-metal-organic framework nanozyme Q-MIL-53(Fe) is reported via a controlled deligandation strategy, exhibiting enhanced peroxidase-/catalase-mimic activity and glutathione depletion capacity, whose underlying mechanisms are studied via density functional theory calculations. Q-MIL-53(Fe) demonstrates biocompatibility and superior antitumor efficacy compared to pristine MIL-53(Fe). It can activate antitumor immune response by inducing ferroptosis and immunogenic cell death, promoting dendritic cell maturation and T lymphocytes infiltration. Furthermore, a combination of Q-MIL-53(Fe) and programmed cell death protein 1 antibody amplifies cancer immunotherapy. This study validates the antitumor activity of quasi-metal-organic frameworks and its immunotherapy induction potential. It would broaden the application of quasi-metal-organic frameworks and open avenues for developing antitumor nanozymes.