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An osmium-peroxo complex for photoactive therapy of hypoxic tumors.

Nong LuZhihong DengJing GaoChao LiangHaiping XiaPingyu Zhang
Published in: Nature communications (2022)
The limited therapeutic effect on hypoxic and refractory solid tumors has hindered the practical application of photodynamic therapy. Herein, we report our investigation of an osmium-peroxo complex (Os2), which is inactive in the dark, but can release a peroxo ligand O 2 •- upon light irradiation even in the absence of oxygen, and is transformed into a cytotoxic osmium complex (Os1). Os1 is cytotoxic in the presence or absence of irradiation in hypoxic tumors, behaving as a chemotherapeutic drug. At the same time, the light-activated Os2 induces photocatalytic oxidation of endogenous 1,4-dihydronicotinamide adenine dinucleotide in living cancer cells, leading to ferroptosis, which is mediated by glutathione degradation, lipid peroxide accumulation and down-regulation of glutathione peroxidase 4. In vivo studies have confirmed that the Os2 can effectively inhibit the growth of solid hypoxic tumors in mice. A promising strategy is proposed for the treatment of hypoxic tumors with metal-based drugs.
Keyphrases
  • photodynamic therapy
  • hydrogen peroxide
  • cell death
  • type diabetes
  • emergency department
  • metabolic syndrome
  • reduced graphene oxide
  • skeletal muscle
  • adipose tissue
  • visible light
  • case control
  • replacement therapy