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氧化铜纳米颗粒通过破坏性自噬诱导增强的放射增敏效应。

Copper Oxide Nanoparticles Induce Enhanced Radiosensitizing Effect via Destructive Autophagy.

作者信息

Jiang Yao-Wen, Gao Ge, Jia Hao-Ran, Zhang Xiaodong, Zhao Jing, Ma Ningning, Liu Jia-Bao, Liu Peidang, Wu Fu-Gen

出版信息

ACS Biomater Sci Eng. 2019 Mar 11;5(3):1569-1579. doi: 10.1021/acsbiomaterials.8b01181. Epub 2019 Feb 20.

DOI:10.1021/acsbiomaterials.8b01181
PMID:33405630
Abstract

Emerging nanotechnologies for radiotherapy are attracting increasing interest from researchers in recent years. To improve the radiotherapeutic performance, developing nanoparticles that can efficiently generate toxic reactive oxygen species (ROS) under X-ray irradiation are highly desirable. Here, we investigate the potential of copper oxide nanoparticles (CuO NPs) as nanoradiosensitizers. Increased cancer cell inhibition is observed in colony formation assay and real-time cell analysis after the combined treatment with CuO NPs and X-ray irradiation, whereas the CuO NPs alone do not have any negative influence on cell viability, indicating the radiosensitization effect of CuO NPs. Importantly, the significantly increased ROS level in cells contributes to the enhanced damage to cancer cells under the combined treatment. Besides, the cell cycle is regulated to the X-ray-sensitive phase (G/M phase) by CuO NPs, which may also account for the inhibited proliferation of cancer cells. Furthermore, results from Western blot analysis and colony formation assay reveal that the increased cell death may be mainly attributed to the excessive autophagy induced by both CuO NPs and X-ray irradiation. Moreover, in vivo experiments verify the radiosensitization of CuO NPs and their favorable biosafety. The current study suggests that CuO NPs can be utilized as nanoradiosensitizers for increasing the efficiency of cancer radiotherapy.

摘要

近年来,用于放射治疗的新兴纳米技术越来越受到研究人员的关注。为了提高放射治疗性能,开发能够在X射线照射下有效产生活性氧(ROS)的纳米颗粒是非常有必要的。在此,我们研究了氧化铜纳米颗粒(CuO NPs)作为纳米放射增敏剂的潜力。在CuO NPs与X射线联合处理后的集落形成试验和实时细胞分析中,观察到癌细胞抑制作用增强,而单独的CuO NPs对细胞活力没有任何负面影响,表明CuO NPs具有放射增敏作用。重要的是,联合处理下细胞内ROS水平显著升高,这有助于增强对癌细胞的损伤。此外,CuO NPs将细胞周期调节至对X射线敏感的阶段(G/M期),这也可能是癌细胞增殖受到抑制的原因。此外,蛋白质印迹分析和集落形成试验结果表明,细胞死亡增加可能主要归因于CuO NPs和X射线照射诱导的过度自噬。此外,体内实验证实了CuO NPs的放射增敏作用及其良好的生物安全性。当前研究表明,CuO NPs可作为纳米放射增敏剂用于提高癌症放射治疗的效率。

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