Suppressing the Radiation-Induced Corrosion of Bismuth Nanoparticles for Enhanced Synergistic Cancer Radiophototherapy.
Ruyi ZhouXinxin LiuYuanzheng WuHuandong XiangJitao CaoYinghao LiWenyan YinYan ZuJinxia LiRu LiuFeng ZhaoZhongdong LiuChunying ChenZhanjun GuYuliang ZhaoYuliang ZhaoPublished in: ACS nano (2020)
The level of tumor killing by bismuth nanoparticles (BiNPs) as radiosensitizers depends strongly on the powerful particle-matter interaction. However, this same radiation leads to the structural damage in BiNPs, consequently weakening their specific physicochemical properties for radiosensitization. Herein, we studied the radiation-induced corrosion behavior of BiNPs and demonstrated that these damages were manifested by the change in their morphology and crystal structure as well as self-oxidation at their surface. Furthermore, artificial heterostructures were created with graphene nanosheets to greatly suppress the radiation-induced corrosion in BiNPs and enhance their radiocatalytic activity for radiotherapy enhancement. Such a nanocomposite allows the accumulation of overexpressed glutathione, a natural hole scavenger, at the reaction interfaces. This enables the rapid removal of radiogenerated holes from the surface of BiNPs and minimizes the self-radiooxidation, therefore resulting in an efficient suppression of radiation corrosion and a decrease of the depletion of reactive oxygen species (ROS). Meanwhile, the radioexcited conduction band electrons react with the high-level H2O2 within cancer cells to yield more ROS, and the secondary electrons are trapped by H2O molecules to produce hydrated electrons capable of reducing a highly oxidized species such as cytochrome c. These radiochemical reactions together with hyperthermia can regulate the tumor microenvironment and accelerate the onset of cellular redox disequilibrium, mitochondrial dysfunction, and DNA damage, finally triggering tumor apoptosis and death. The current work will shed light on radiosensitizers with an enhanced corrosion resistance for controllable and synergistic radio-phototherapeutics.
Keyphrases
- radiation induced
- dna damage
- reactive oxygen species
- radiation therapy
- oxidative stress
- crystal structure
- visible light
- cell death
- reduced graphene oxide
- quantum dots
- dna repair
- papillary thyroid
- signaling pathway
- walled carbon nanotubes
- carbon nanotubes
- squamous cell
- early stage
- cell proliferation
- cell cycle arrest
- hydrogen peroxide
- electron transfer
- lymph node metastasis
- high resolution
- young adults
- sensitive detection