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The fate of ZnO nanoparticles administered to human bronchial epithelial cells

机译:ZnO纳米颗粒对人支气管上皮细胞的命运

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Figure Persented: A particular challenge for nanotoxicology is the evaluation of the biological fate and toxicity of nanomaterials that dissolve in aqueous fluids. Zinc oxide nanomaterials are of particular concern because dissolution leads to release of the toxic divalent zinc ion. Although zinc ions have been implicated in ZnO cytotoxicity, direct identification of the chemical form of zinc taken up by cells exposed to ZnO nanoparticles, and its intracellular fate, has not yet been achieved. We combined high resolution X-ray spectromicroscopy and high elemental sensitivity X-ray microprobe analyses to determine the fate of ZnO and less soluble iron-doped ZnO nanoparticles following exposure to cultures of human bronchial epithelial cells, BEAS-2B. We complemented two-dimensional X-ray imaging methods with atomic force microscopy of cell surfaces to distinguish between nanoparticles that were transported inside the cells from those that adhered to the cell exterior. The data suggest cellular uptake of ZnO nanoparticles is a mechanism of zinc accumulation in cells. Following uptake, ZnO nanoparticles dissolved completely generating intracellular Zn 2+ complexed by molecular ligands. These results corroborate a model for ZnO nanoparticle toxicity that is based on nanoparticle uptake followed by intracellular dissolution.
机译:可能的图:纳米毒理学的一个特殊挑战是评估溶于水性液体的纳米材料的生物命运和毒性。氧化锌纳米材料特别受关注,因为溶解导致有毒二价锌离子的释放。尽管锌离子与ZnO的细胞毒性有关,但尚未直接鉴定暴露于ZnO纳米颗粒的细胞吸收的锌的化学形式及其细胞内命运。我们将高分辨率X射线光谱显微镜和高元素敏感性X射线显微探针分析相结合,以确定暴露于人支气管上皮细胞BEAS-2B培养物中的ZnO和难溶的铁掺杂ZnO纳米颗粒的命运。我们用细胞表面的原子力显微镜对二维X射线成像方法进行了补充,以区分在细胞内部运输的纳米颗粒和粘附在细胞外部的纳米颗粒。数据表明细胞摄取ZnO纳米颗粒是锌在细胞中积累的机制。摄取后,ZnO纳米颗粒完全溶解,生成分子内配体复合的细胞内Zn 2+。这些结果证实了基于纳米颗粒摄取随后细胞内溶解的ZnO纳米颗粒毒性模型。

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