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首页> 外文期刊>ACS nano >High-Content Imaging and Gene Expression Approaches To Unravel the Effect of Surface Functionality on Cellular Interactions of Silver Nanoparticles
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High-Content Imaging and Gene Expression Approaches To Unravel the Effect of Surface Functionality on Cellular Interactions of Silver Nanoparticles

机译:高内涵成像和基因表达方法,揭示表面功能对银纳米粒子细胞相互作用的影响

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The toxic effects of Ag nanoparticles (NPs) remain an issue of debate, where the respective contribution of the NPs themselves and of free Ag+ ions present in the NP stock suspensions and after intracellular NP corrosion are not fully understood. Here, we employ a recently set up methodology based on high-content (HC) imaging combined with high-content gene expression studies to examine the interaction of three types of Ag NPs with identical core sizes, but coated with either mercaptoundecanoic acid (MUA), dodecylamine-modified poly(isobutylene-alt-maleic anhydride) (PMA), or poly(ethylene glycol) (PEG)-conjugated PMA with two types of cultured cells (primary human umbilical vein endothelial cells (HUVEC) and murine C17.2 neural progenitor cells). As a control, cells were also exposed to free Ag+ ions at the same concentration as present in the respective Ag NP stock suspensions. The data reveal clear effects of the NP surface properties on cellular interactions. PEGylation of the NPs significantly reduces their cellular uptake efficiency, whereas MUA-NPs are more prone to agglomeration in complex tissue culture media. PEG-NPs display the lowest levels of toxicity, which is in line with their reduced cell uptake. MUA-NPs display the highest levels of toxicity, caused by autophagy, cell membrane damage, mitochondrial damage, and cytoskeletal deformations. At similar intracellular NP levels, PEG-NPs induce the highest levels of reactive oxygen species (ROS), but do not affect the cell cytoskeleton, in contrast to MUA- and PMA-NPs. Gene expression studies support the findings above, defining autophagy and cell membrane damage-related necrosis as main toxicity pathways. Additionally, immunotoxicity, DNA damage responses, and hypoxia-like toxicity were observed for PMA- and especially MUA-NPs. Together, these data reveal that Ag+ ions do contribute to Ag NP-associated toxicity, particularly upon intracellular degradation. The different surface properties of the NPs however result in distinct toxicity profiles for the three NPs, indicating clear NP-associated effects.
机译:Ag纳米颗粒(NPs)的毒性作用仍是一个有争议的问题,其中对NPs本身以及NP储液悬浮液中以及细胞内NP腐蚀后存在的游离Ag +离子的各自贡献尚不完全清楚。在这里,我们采用了基于高含量(HC)成像和高含量基因表达研究的最新建立的方法,以检查三种具有相同核大小但涂有巯基癸酸(MUA)的Ag NP的相互作用,十二烷基胺修饰的聚(异丁烯-马来酸酐)(PMA)或聚(乙二醇)(PEG)偶联的PMA,具有两种类型的培养细胞(原代人脐静脉内皮细胞(HUVEC)和鼠C17.2神经祖细胞)。作为对照,还将细胞暴露于游离Ag +离子,其浓度与相应的Ag NP储备悬浮液中存在的浓度相同。数据揭示了NP表面性质对细胞相互作用的明显影响。 NP的聚乙二醇化显着降低了它们的细胞摄取效率,而MUA-NP在复杂的组织培养基中更易于聚集。 PEG-NPs显示出最低的毒性水平,这与它们减少的细胞摄取一致。 MUA-NPs表现出最高的毒性水平,这是由于自噬,细胞膜损伤,线粒体损伤和细胞骨架变形引起的。与MUA-和PMA-NP相比,在相似的细胞内NP水平下,PEG-NPs诱导出最高水平的活性氧(ROS),但不影响细胞的细胞骨架。基因表达研究支持上述发现,将自噬和与细胞膜损伤相关的坏死定义为主要毒性途径。另外,对于PMA-尤其是MUA-NP,观察到了免疫毒性,DNA损伤反应和低氧样毒性。这些数据加在一起表明,Ag +离子确实会导致与Ag NP相关的毒性,特别是在细胞内降解时。但是,NP的不同表面性质导致三种NP具有不同的毒性,表明明显的NP相关作用。

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