What question did this study set out to answer?

The aim is to develop a safer and more effective cancer treatment using glucose oxidase-powered ferrium MOFs.

May 8, 2026

Glucose Oxidase‐Powered Ferrium MOFs for Self‐Amplifying Fenton Catalysis and Photothermal Therapy

Key Points

The aim is to develop a safer and more effective cancer treatment using glucose oxidase-powered ferrium MOFs.
Utilized FHMGA for self-amplifying Fenton catalysis and photothermal therapy.
Investigated the synergistic effects on cancer cell growth inhibition.
Assessed systemic toxicity parameters.
FHMGA significantly inhibits cancer cell growth by leveraging oxidative damage, thermal ablation, and metabolic disruption.
Minimal systemic toxicity observed during treatment across the tested models.
Enhanced tumor-specific treatment achieved without traditional chemotherapy.

Abstract

, further boosting Fenton-like reactions. Our results demonstrate that FHMGA exhibits significant anti-tumor efficacy with minimal systemic toxicity. The triple synergy of oxidative damage from chemodynamic therapy, thermal ablation from photothermal therapy, and metabolic disruption via glucose oxidase significantly inhibits cancer cell growth by overcoming antioxidant-mediated limitations. Self-amplifying Fenton catalysis, while responsive degradation reduces systemic toxicity. This work advances precise cancer therapy by establishing a chemotherapy-free, multi-responsive synergistic system, addressing critical bottlenecks of ferrium-based MOFs and providing a safer, more effective strategy for tumor-specific treatment.

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Cite This Study

Xin et al. (Wed,) studied this question.

synapsesocial.com/papers/69fd7e79bfa21ec5bbf06b79 https://doi.org/https://doi.org/10.1002/adhm.71190

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