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铁掺杂氧化铜纳米粒子降低其对 C6 神经胶质瘤细胞的毒性。

Iron-Doping of Copper Oxide Nanoparticles Lowers Their Toxic Potential on C6 Glioma Cells.

机构信息

Center for Biomolecular Interactions Bremen, Faculty 2 (Biology/Chemistry), University of Bremen, PO. Box 330440, 28334, Bremen, Germany.

Center for Environmental Research and Sustainable Technology, Leobener Strasse 5, 28359, Bremen, Germany.

出版信息

Neurochem Res. 2020 Apr;45(4):809-824. doi: 10.1007/s11064-020-02954-y. Epub 2020 Jan 29.

Abstract

Copper oxide nanoparticles (CuO-NPs) are well known for their cytotoxicity which in part has been attributed to the release of copper ions from CuO-NPs. As iron-doping has been reported to reduce the susceptibility of CuO-NPs to dissolution, we have compared pure CuO-NPs and CuO-NPs that had been doped with 10% iron (CuO-Fe-NPs) for copper release and for their toxic potential on C6 glioma cells. Physicochemical characterization revealed that dimercaptosuccinate (DMSA)-coated CuO-NPs and CuO-Fe-NPs did not differ in their size or zeta potential. However, the redox activity and liberation of copper ions from CuO-Fe-NPs was substantially slower compared to that from CuO-NPs, as demonstrated by cyclic voltammetry and by the photometric quantification of the copper ion-bathocuproine complex, respectively. Exposure of C6 cells to these NPs caused an almost identical cellular copper accumulation and each of the two types of NPs induced ROS production and cell toxicity. However, the time- and concentration-dependent loss in cell viability was more severe for cells that had been treated with CuO-NPs compared to cells exposed to CuO-Fe-NPs. Copper accumulation and toxicity after exposure to either CuO-NPs or CuO-Fe-NPs was prevented in the presence of copper chelators, while neutralization of the lysosomal pH by bafilomycin A1 prevented toxicity without affecting cellular copper accumulation or ROS production. These data demonstrate that iron-doping does not affect cellular accumulation of CuO-NPs and suggests that the intracellular liberation of copper ions from CuO-NPs is slowed by the iron doping, which in turn lowers the cell toxic potential of iron-doped CuO-NPs.

摘要

氧化铜纳米颗粒 (CuO-NPs) 以其细胞毒性而闻名,部分原因是 CuO-NPs 释放出铜离子。由于铁掺杂已被报道可降低 CuO-NPs 的溶解敏感性,因此我们比较了纯 CuO-NPs 和掺杂了 10%铁的 CuO-NPs (CuO-Fe-NPs) 的铜释放和对 C6 神经胶质瘤细胞的毒性潜力。物理化学特性分析表明,二巯丁二酸 (DMSA) 包裹的 CuO-NPs 和 CuO-Fe-NPs 在粒径和zeta 电位方面没有差异。然而,循环伏安法和分光光度法定量测定铜离子-铜试剂络合物分别表明,CuO-Fe-NPs 的氧化还原活性和铜离子的释放速度明显比 CuO-NPs 慢。这些 NPs 暴露于 C6 细胞中会导致几乎相同的细胞内铜积累,并且这两种类型的 NPs 均会诱导 ROS 产生和细胞毒性。然而,与暴露于 CuO-Fe-NPs 的细胞相比,用 CuO-NPs 处理的细胞的细胞活力随时间和浓度依赖性下降更为严重。在用铜螯合剂处理后,无论是暴露于 CuO-NPs 还是 CuO-Fe-NPs 后,细胞内铜积累和毒性都得到了预防,而通过 bafilomycin A1 中和溶酶体 pH 可以预防毒性,而不会影响细胞内铜积累或 ROS 产生。这些数据表明,铁掺杂不会影响 CuO-NPs 的细胞积累,并表明铁掺杂降低了 CuO-NPs 从细胞内释放铜离子的速度,从而降低了铁掺杂的 CuO-NPs 的细胞毒性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/118d/7078150/06282e199455/11064_2020_2954_Fig1_HTML.jpg

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