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Enhanced cytotoxic and genotoxic effects of gadolinium-doped ZnO nanoparticles on irradiated lung cancer cells at megavoltage radiation energies

机译:掺杂的ZnO纳米颗粒对兆伏级辐射能量下照射的肺癌细胞具有增强的细胞毒性和遗传毒性作用

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The purpose of this study was to investigate the radiation dose enhancement effects of gadolinium-doped zinc oxide nanoparticles (Gd-doped ZnO NPs) under the megavoltage (MV) X-ray irradiation. ZnO NPs have preferred photocatalytic properties under UV light for cancer killing. UV light has limited applications in cancer treatment and it is necessary to use X-ray photons with MV energies. In order to increase the absorption of radiation and also to enhance the imaging visualization capabilities of ZnO NPs, gadolinium (Gd) as a high atomic number element was selected for doping into the structure of ZnO NPs. Gd-doped ZnO NPs were synthesized by a chemical precipitation method and characterized by transmission electron microscopy, powder X-ray diffraction, ultraviolet-visible spectroscopy, and energy-dispersive X-ray techniques. Cellular uptake was assessed by TEM and inductively coupled plasma mass spectrometry. NPs cytotoxicity was analyzed by MTT assay and radiation dose enhancement was measured by clonogenic survival assay. Apoptosis induction, cell cycle progression, micronucleus formation and expression of DNA double-strand break repair genes of XRCC2 and XRCC4 were determined by flow cytometry, micronucleus assay, and quantitative real-time polymerase chain reaction. CT and MR imaging were used to analyze the image visualization capabilities of NPs. NPs characterization showed that highly pure crystalline Gd-doped ZnO NPs with a narrow size distribution and grain size of 9 nm were synthesized. Gd-doped ZnO NPs were distributed in the cells and showed dose-dependent toxicity. Combination of Gd-doped ZnO NPs with 6 MV X-rays induced dose-dependent radiosensitivity with sensitizer enhancement ratios (SER) of 1.47 and 1.61 for 10 and 20 mu g/mL NPs concentrations. Cancer cells blocked in Gl, apoptosis rates, and micronuclei formation was enhanced and inversely, the DNA repair efficiency was impaired by down regulation of the mRNA levels of XRCC2 and XRCC4 genes. Gd-doped ZnO NPs enhanced the contrasts of CT and MR images of cancer cells. Overall, the results of this study provide detailed biological insights on the dose enhancement of Gd-doped ZnO NPs at MV radiations, which would contribute to the further development of this potent theranostic platform for clinical applications.
机译:这项研究的目的是研究在高电压(MV)X射线辐射下掺ado的氧化锌纳米颗粒(掺Gd的ZnO NPs)的辐射剂量增强作用。 ZnO NP在紫外线下具有较好的光催化特性,可杀死癌症。紫外线在癌症治疗中的应用受到限制,因此必须使用具有MV能量的X射线光子。为了增加辐射的吸收并增强ZnO NP的成像可视化能力,选择了as(Gd)作为高原子序数元素掺杂到ZnO NPs的结构中。 precipitation掺杂的ZnO纳米粒子是通过化学沉淀法合成的,并通过透射电子显微镜,粉末X射线衍射,紫外可见光谱和能量色散X射线技术表征。通过TEM和电感耦合等离子体质谱法评估细胞摄取。通过MTT分析法分析NP的细胞毒性,并通过克隆形成存活分析法测量辐射剂量的增加。通过流式细胞仪,微核分析和定量实时聚合酶链反应测定XRCC2和XRCC4的凋亡诱导,细胞周期进程,微核形成和DNA双链断裂修复基因的表达。 CT和MR成像用于分析NP的图像可视化功能。 NPs表征表明,合成了具有窄尺寸分布和9 nm晶粒尺寸的高纯Gd掺杂ZnO NPs NP。 Gd掺杂的ZnO NPs分布在细胞中,并显示出剂量依赖性毒性。 Gd掺杂的ZnO NP与6 MV X射线的组合可诱导剂量依赖性放射敏感性,其中10和20μg / mL NPs浓度的增感剂增强比(SER)为1.47和1.61。反之,通过下调XRCC2和XRCC4基因的mRNA水平,癌细胞在G1中受阻,凋亡率和微核形成被增强,并且相反地,DNA修复效率受到损害。 Gd掺杂的ZnO NP增强了癌细胞CT和MR图像的对比度。总体而言,这项研究的结果提供了在MV辐射下掺Gd掺杂的ZnO NPs剂量增加的详细生物学见解,这将有助于进一步开发这种强大的临床治疗平台。

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