FeS 2 -modified MXene nanocomposite platform for efficient PTT/CDT/TDT integration through enhanced GSH consumption.
Yunfeng TangRenliang ZhaoMin YiZilu GeDong WangYu JiangGuanglin WangXiangtian DengPublished in: Journal of materials chemistry. B (2024)
Hypoxic microenvironment and glutathione (GSH) accumulation in tumours limit the efficacy of cytotoxic reactive oxygen species (ROS) anti-tumour therapy. To address this challenge, we increased the consumption of GSH and the production of ROS through a novel nanoplatform with the action of inorganic nanoenzymes. In this study, we prepared mesoporous FeS 2 using a simple template method, efficiently loaded AIPH, and assembled Ti 3 C 2 /FeS 2 -AIPH@BSA (TFAB) nanocomposites through self-assembly with BSA and 2D Ti 3 C 2 . The constructed TFAB nanotherapeutic platform enhanced chemodynamic therapy (CDT) by generating toxic hydroxyl radicals (˙OH) via FeS 2 , while consuming GSH to reduce the loss of generated ˙OH via glutathione oxidase-like (GSH-OXD). In addition, TFAB is able to stimulate the decomposition of AIPH under 808 nm laser irradiation to produce oxygen-independent biotoxic alkyl radicals (˙R) for thermodynamic therapy (TDT). In conclusion, TFAB represents an innovative nanoplatform that effectively addresses the limitations of free radical-based treatment strategies. Through the synergistic therapeutic strategy of photothermal therapy (PTT), CDT, and TDT within the tumor microenvironment, TFAB nanoplatforms achieve controlled AIPH release, ROS generation, intracellular GSH consumption, and precise temperature elevation, resulting in enhanced intracellular oxidative stress, significant apoptotic cell death, and notable tumor growth inhibition. This comprehensive treatment strategy shows great promise in the field of tumor therapy.
Keyphrases
- cell death
- reactive oxygen species
- fluorescent probe
- dna damage
- oxidative stress
- cancer therapy
- photodynamic therapy
- drug delivery
- stem cells
- high throughput
- high resolution
- mesenchymal stem cells
- cell therapy
- ischemia reperfusion injury
- quantum dots
- radiation induced
- drug release
- induced apoptosis
- water soluble
- heat shock