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首页> 外文期刊>Nanoscale >An automatable platform for genotoxicity testing of nanomaterials based on the fluorometric gamma-H2AX assay reveals no genotoxicity of properly surface-shielded cadmium-based quantum dots
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An automatable platform for genotoxicity testing of nanomaterials based on the fluorometric gamma-H2AX assay reveals no genotoxicity of properly surface-shielded cadmium-based quantum dots

机译:可自动化的基因毒性测试平台基于纳米材料的荧光gamma-H2AX化验的基因毒性正确surface-shielded cadmium-based量子点

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摘要

The large number of nanomaterial-based applications emerging in the materials and life sciences and the foreseeable increasing use of these materials require methods that evaluate and characterize the toxic potential of these nanomaterials to keep safety risks to people and environment as low as possible. As nanomaterial toxicity is influenced by a variety of parameters like size, shape, chemical composition, and surface chemistry, high throughput screening (HTS) platforms are recommended for assessing cytotoxicity. Such platforms are not yet available for genotoxicity testing. Here, we present first results obtained for application-relevant nanomaterials using an automatable genotoxicity platform that relies on the quantification of the phosphorylated histone H2AX (gamma-H2AX) for detecting DNA double strand breaks (DSBs) and the automated microscope system AKLIDES (R) for measuring integral fluorescence intensities at different excitation wavelengths. This platform is used to test the genotoxic potential of 30 nm-sized citrate-stabilized gold nanoparticles (Au-NPs) as well as micellar encapsulated iron oxide nanoparticles (FeOx-NPs) and different cadmium (Cd)-based semiconductor quantum dots (QDs), thereby also searching for positive and negative controls as reference materials. In addition, the influence of the QD shell composition on the genotoxic potential of these Cd-based QDs was studied, using CdSe cores as well as CdSe/CdS core/shell and CdSe/CdS/ZnS core/shell/shell QDs. Our results clearly revealed the genotoxicity of the Au-NPs and its absence in the FeOx-NPs. The genotoxicity of the Cd-QDs correlates with the shielding of their Cd-containing core, with the core/shell/shell architecture preventing genotoxicity risks. The fact that none of these nanomaterials showed cytotoxicity at the chosen particle concentrations in a conventional cell viability assay underlines the importance of genotoxicity studies to assess the hazardous potential of nanomaterials.
机译:大量的nanomaterial-based应用新兴材料和生活科学和可预见的使用增加这些材料需要评估和方法描述的潜在毒性纳米材料使人们和安全风险环境尽可能低。毒性是受各种参数的影响如大小、形状、化学成分和表面化学、高通量筛选(高温超导)平台推荐的评估细胞毒性。用于基因毒性测试。第一个结果application-relevant纳米材料使用可自动化的基因毒性依赖的平台磷酸化的量化组蛋白H2AX (gamma-H2AX)检测DNA双链休息(双边带)和自动显微镜系统AKLIDES (R)测量荧光积分在不同激发波长的强度。这个平台是用来测试基因毒性潜在的30 nm-sized citrate-stabilized黄金纳米颗粒(Au-NPs)以及胶束封装的氧化铁纳米颗粒(FeOx-NPs)和不同镉(Cd)的半导体量子点(量子点),从而也在寻找积极的和消极的控制参考材料。壳组成的基因毒性的潜力这些制作基于量子点研究,使用CdSe内核以及CdSe核/壳和CdSe / CdS / cd /硫化锌核/壳量子点/壳。揭示了Au-NPs及其基因毒性FeOx-NPs缺席。Cd-QDs与他们的屏蔽cd片核心,核心/壳壳体系结构防止基因毒性的风险。这些纳米材料显示的事实选择粒子的细胞毒性浓度在传统细胞生存能力分析突显出基因毒性的重要性研究,以评估潜在的危险纳米材料。

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