Reactive Oxygen Species Amplifier for Apoptosis-Ferroptosis Mediated High-Efficiency Radiosensitization of Tumors

活性氧 细胞凋亡 DNA损伤 电离辐射 癌症研究 抗辐射性 材料科学 脂质过氧化 纳米探针 氧化应激 生物物理学 化学 生物 细胞生物学 纳米技术 放射治疗 DNA 辐照 医学 生物化学 物理 内科学 纳米颗粒 核物理学
作者
Ze Wang,Xiaojun Ren,Yunfeng Li,Ling Qiu,Dongzhou Wang,Annan Liu,Hao Liang,Lei Li,Bai Yang,Andrew K. Whittaker,Zhongshan Liu,Shunzi Jin,Quan Lin,Zhihui Wang
出处
期刊:ACS Nano [American Chemical Society]
卷期号:18 (14): 10288-10301 被引量:1
标识
DOI:10.1021/acsnano.4c01625
摘要

Insufficient reactive oxygen species (ROS) production and radioresistance have consistently contributed to the failure of radiotherapy (RT). The development of a biomaterial capable of activating ROS-induced apoptosis and ferroptosis is a potential strategy to enhance RT sensitivity. To achieve precision and high-efficiency RT, the theranostic nanoplatform Au/Cu nanodots (Au/CuNDs) were designed for dual-mode imaging, amplifying ROS generation, and inducing apoptosis-ferroptosis to sensitize RT. A large amount of ROS is derived from three aspects: (1) When exposed to ionizing radiation, Au/CuNDs effectively absorb photons and emit various electrons, which can interact with water to produce ROS. (2) Au/CuNDs act as a catalase-like to produce abundant ROS through Fenton reaction with hydrogen peroxide overexpressed of tumor cells. (3) Au/CuNDs deplete overexpressed glutathione, which causes the accumulation of ROS. Large amounts of ROS and ionizing radiation further lead to apoptosis by increasing DNA damage, and ferroptosis by enhancing lipid peroxidation, significantly improving the therapeutic efficiency of RT. Furthermore, Au/CuNDs serve as an excellent nanoprobe for high-resolution near-infrared fluorescence imaging and computed tomography of tumors. The promising dual-mode imaging performance shows their potential application in clinical cancer detection and imaging-guided precision RT, minimizing damage to adjacent normal tissues during RT. In summary, our developed theranostic nanoplatform integrates dual-mode imaging and sensitizes RT via ROS-activated apoptosis-ferroptosis, offering a promising prospect for clinical cancer diagnosis and treatment.
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