Fe 3 O 4 @TiO 2 Microspheres: Harnessing O 2 Release and ROS Generation for Combination CDT/PDT/PTT/Chemotherapy in Tumours.
Bo ZhaoXiuli HuLu ChenXin WuDonghui WangHongshui WangChunyong LiangPublished in: Nanomaterials (Basel, Switzerland) (2024)
In the treatment of various cancers, photodynamic therapy (PDT) has been extensively studied as an effective therapeutic modality. As a potential alternative to conventional chemotherapy, PDT has been limited due to the low Reactive Oxygen Species (ROS) yield of photosensitisers. Herein, a nanoplatform containing mesoporous Fe 3 O 4 @TiO 2 microspheres was developed for near-infrared (NIR)-light-enhanced chemodynamical therapy (CDT) and PDT. Titanium dioxide (TiO 2 ) has been shown to be a very effective PDT agent; however, the hypoxic tumour microenvironment partly affects its in vivo PDT efficacy. A peroxidase-like enzyme, Fe 3 O 4 , catalyses the decomposition of H 2 O 2 in the cytoplasm to produce O 2 , helping overcome tumour hypoxia and increase ROS production in response to PDT. Moreover, Fe 2+ in Fe 3 O 4 could catalyse H 2 O 2 decomposition to produce cytotoxic hydroxyl radicals within tumour cells, which would result in tumour CDT. The photonic hyperthermia of Fe 3 O 4 @TiO 2 could not only directly damage the tumour but also improve the efficiency of CDT from Fe 3 O 4 . Cancer-killing effectiveness has been maximised by successfully loading the chemotherapeutic drug DOX, which can be released efficiently using NIR excitation and slight acidification. Moreover, the nanoplatform has high saturation magnetisation (20 emu/g), making it suitable for magnetic targeting. The in vitro results show that the Fe 3 O 4 @TiO 2 /DOX nanoplatforms exhibited good biocompatibility as well as synergetic effects against tumours in combination with CDT/PDT/PTT/chemotherapy.
Keyphrases
- photodynamic therapy
- reactive oxygen species
- fluorescence imaging
- visible light
- quantum dots
- cell death
- systematic review
- locally advanced
- induced apoptosis
- randomized controlled trial
- molecularly imprinted
- multidrug resistant
- cell cycle arrest
- endothelial cells
- risk assessment
- squamous cell carcinoma
- hydrogen peroxide
- mesenchymal stem cells
- signaling pathway
- human health
- rectal cancer
- emergency department
- young adults
- cell therapy
- squamous cell
- metal organic framework
- endoplasmic reticulum stress
- adverse drug
- energy transfer