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Blocking glutathione regeneration: Inorganic NADPH oxidase nanozyme catalyst potentiates tumoral ferroptosis

Nano Today, ISSN: 1748-0132, Vol: 46, Page: 101574
2022
  • 83
    Citations
  • 0
    Usage
  • 18
    Captures
  • 1
    Mentions
  • 0
    Social Media
Metric Options:   Counts1 Year3 Year

Metrics Details

  • Citations
    83
    • Citation Indexes
      83
  • Captures
    18
  • Mentions
    1
    • News Mentions
      1
      • News
        1

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Introduction Breast cancer (BC) stands as one of the most frequently diagnosed cancers among females globally.1 In clinical practice, a combination of surgery, chemotherapy, and

Article Description

Emerging cancer cell ferroptosis features the direct depletion of glutathione (GSH) and resultant chemical inhibition on glutathione peroxidase 4 (GPX4) bioactivity, which, unfortunately, is counteracted considerably by nicotinamide adenine dinucleotide phosphate (NADPH)-enabled regeneration of antioxidant GSH. Herein, a Pt-MIL-101 (Fe)-based nanocatalytic medicine (NCM) is proposed to catalyze NADPH oxidation and the following nanozyme catalytic cascade reactions to produce hydroxyl radicals and prevent GSH regeneration, thus promoting the ferroptotic death of cancer cells. Briefly, the Pt-MIL-101 nanomedicine possessing NADPH oxidase (NOX)-like activity catalyzes the superoxide anions (O 2 •− ) generation by promoting the electron transfer from NADPH to O 2, followed by Pt-MIL-101-catalyzed O 2 •− disproportionation producing H 2 O 2 using its superoxide dismutase (SOD) nanozyme catalytic activity. The generated H 2 O 2 further serves as substrate for toxic ∙OH production via Fenton reaction with Fe 3+ /Fe 2+ at the structure center of the MIL-101. Moreover, the NOX nanozyme-catalyzed NADPH depletion by the nanomedicine largely prevents the GSH regeneration and de-activates GPX4, promoting lipid peroxidation for ferroptotic cell death. This work highlights an effective NADPH-initiated nanozyme cascade nanocatalytic strategy for ferroptosis-based tumor therapy.

Bibliographic Details

Chenyao Wu; Deliang Xu; Min Ge; Juanjuan Luo; Lisong Chen; Zhixin Chen; Yanling You; Ya-xuan Zhu; Han Lin; Jianlin Shi

Elsevier BV

Biochemistry, Genetics and Molecular Biology; Chemical Engineering; Engineering; Materials Science; Pharmacology, Toxicology and Pharmaceutics

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