Tumor Microenvironment-Activated
In Situ Synthesis
of Peroxynitrite for Enhanced Chemodynamic Therapy
Posted on 2024-09-19 - 16:33
Chemodynamic therapy (CDT) can induce cancer cell death
through
hydroxyl radicals (·OH) generated from Fenton or Fenton-like
reactions. Compared with traditional therapies, CDT effectively overcomes
inevitable drug resistance and exhibits low side effects. However,
clinical application still faces challenges, primarily due to insufficient
·OH generation and the short-lifetime of ·OH in vivo. To
address these challenges, we developed a peroxynitrite (ONOO–)-based CDT nanodrug (DOX@PMOF) composed of MOF-199, NO donor (PArg),
and nicotinamide adenine dinucleotide phosphate oxidase 4 (NOX4) activator
(doxorubicin, DOX). In DOX@PMOF, MOF-199 serves as both a carrier
for loading DOX and a source of Cu+ for triggering CDT.
Upon uptake by cancer cells, the high concentration of glutathione
(GSH) reduces MOF-199 to Cu+, which then reacts with H2O2 to generate ·OH. Moreover, the released
DOX upregulates NOX4 expression, leading to the elevated H2O2 level and thereby promoting a high-efficiency Fenton-like
reaction for sufficient ·OH generation. Subsequently, PArg generates
abundant NO in response to the tumor microenvironment, leading to
a cascade of NO and ·OH for the in situ synthesis of ONOO–. ONOO– is more toxic and has a longer
lifetime and diffusion distance than ·OH, resulting in a more
effective CDT treatment. To further enhance the in vivo therapeutic
effect, we coated DOX@PMOF with a homologous cell membrane to form
an active tumor-targeting nanodrug (DOX@MPMOF), which has demonstrated
the ability to effectively inhibit tumor growth and metastasis while
exhibiting good biosafety.
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Li, Bowen; Wu, Chongzhi; Li, Zhiyao; Yao, Zhuo; Tian, Jianwu; Shan, Yi; et al. (2024). Tumor Microenvironment-Activated
In Situ Synthesis
of Peroxynitrite for Enhanced Chemodynamic Therapy. ACS Publications. Collection. https://doi.org/10.1021/acsnano.4c10012