Glutathione-Triggered catalytic response of Copper-Iron mixed oxide Nanoparticles. Leveraging tumor microenvironment conditions for chemodynamic therapy

https://doi.org/10.1016/j.jcis.2022.03.036Get rights and content
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Abstract

Heterogeneous catalysis has emerged as a promising alternative for the development of new cancer therapies. In addition, regarding the tumor microenvironment as a reactor with very specific chemical features has provided a new perspective in the search for catalytic nanoarchitectures with specific action against chemical species playing a key role in tumor metabolism. One of these species is glutathione (GSH), whose depletion is the cornerstone of emerging strategies in oncology, since this metabolite plays a pivotal regulatory role as antioxidant agent, dampening the harmful effects of intracellular reactive oxidative species (ROS). Herein, we present copper-iron oxide spinel nanoparticles that exhibit a versatile and selective catalytic response to reduce GSH levels while generating ROS in a cascade reaction. We demonstrate a clear correlation between GSH depletion and apoptotic cell death in tumor cells in the presence of the copper-iron nanocatalyst. Furthermore, we also provide a novel analytical protocol, alternative to state-of-the-art commercial kits, to accurately monitoring the concentration of GSH intracellular levels in both tumor and healthy cells. We observe a selective action of the nanoparticles, with lower toxicity in healthy cell lines, whose intrinsic GSH levels are lower, and intense apoptosis in tumor cells accompanied by a fast reduction of GSH levels.

Graphical abstract

Bringing Glutathione down: Copper-Iron based nanoparticles play a determining catalytic role to favor Glutathione (GSH) depletion and subsequently generate reactive oxidative species (ROS) that pave the way for a promising ChemoDynamic Therapy based on the selective overexpression of redox active molecules especially in cancer cells.

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Keywords

Nanocatalysis
Cancer Therapy
Reactive Oxidative Species
Fenton reactions
Glutathione
Cascade Reactions

Abbreviations

GSH
Glutathione
ROS
Reactive Oxygen Species
TME
Tumor Microenvironment
CDT
Chemodynamic Therapy
GPX4
Glutathione Peroxidase
hpMSC
Human Placental Mesenchymal Stem Cells

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These authors contributed equally to this work.