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含铜纳米颗粒诱导的细胞膜损伤和蛋白质相互作用——金属释放过程的重要性。

Cell membrane damage and protein interaction induced by copper containing nanoparticles--importance of the metal release process.

机构信息

Division of Molecular Toxicology, Institute of Environmental Medicine, Karolinska Institutet, Stockholm, Sweden.

出版信息

Toxicology. 2013 Nov 8;313(1):59-69. doi: 10.1016/j.tox.2013.07.012. Epub 2013 Jul 26.

Abstract

Cu-containing nanoparticles are used in various applications in order to e.g. achieve antimicrobial activities and to increase the conductivity of fluids and polymers. Several studies have reported on toxic effects of such particles but the mechanisms are not completely clear. The aim of this study was to investigate the interactions between cell membranes and well-characterized nanoparticles of CuO, Cu metal, a binary Cu-Zn alloy and micron-sized Cu metal particles. This was conducted via in vitro investigations of the effects of the nanoparticles on (i) cell membrane damage on lung epithelial cells (A549), (ii) membrane rupture of red blood cells (hemolysis), complemented by (iii) nanoparticle interaction studies with a model lipid membrane using quartz crystal microbalance with dissipation monitoring (QCM-D). The results revealed that nanoparticles of the Cu metal and the Cu-Zn alloy were both highly membrane damaging and caused a rapid (within 1h) increase in membrane damage at a particle mass dose of 20 μg/mL, whereas the CuO nanoparticles and the micron-sized Cu metal particles showed no such effect. At similar nanoparticle surface area doses, the nano and micron-sized Cu particles showed more similar effects. The commonly used LDH (lactate dehydrogenase) assay for analysis of membrane damage was found impossible to use due to nanoparticle-assay interactions. None of the particles induced any hemolytic effects on red blood cells when investigated up to high particle concentrations (1mg/mL). However, both Cu and Cu-Zn nanoparticles caused hemoglobin aggregation/precipitation, a process that would conceal a possible hemolytic effect. Studies on interactions between the nanoparticles and a model membrane using QCM-D indicated a small difference between the investigated particles. Results of this study suggest that the observed membrane damage is caused by the metal release process at the cell membrane surface and highlight differences in reactivity between metallic nanoparticles of Cu and Cu-Zn and nanoparticles of CuO.

摘要

含铜纳米颗粒在各种应用中被使用,例如实现抗菌活性和提高流体和聚合物的导电性。已有几项研究报告了此类颗粒的毒性作用,但机制尚不完全清楚。本研究的目的是研究细胞与经过良好表征的氧化铜 (CuO)、铜金属、二元铜锌合金和微米级铜金属纳米颗粒之间的相互作用。这是通过体外研究纳米颗粒对(i)肺上皮细胞 (A549) 细胞膜损伤的影响、(ii)红细胞膜破裂(溶血),并辅以(iii)使用石英晶体微天平耗散监测 (QCM-D) 研究纳米颗粒与模型脂质膜的相互作用来进行的。结果表明,铜金属和铜锌合金的纳米颗粒均对细胞膜具有高度破坏性,并在 20μg/mL 颗粒质量剂量下导致细胞膜损伤迅速(在 1 小时内)增加,而 CuO 纳米颗粒和微米级铜金属颗粒则没有这种作用。在类似的纳米颗粒表面积剂量下,纳米和微米级铜颗粒表现出更相似的作用。常用的用于分析细胞膜损伤的 LDH(乳酸脱氢酶)测定法由于纳米颗粒与测定法相互作用而无法使用。当研究高达高颗粒浓度(1mg/mL)时,没有一种颗粒对红细胞产生任何溶血作用。然而,Cu 和 Cu-Zn 纳米颗粒均导致血红蛋白聚集/沉淀,这一过程可能掩盖了可能的溶血作用。使用 QCM-D 研究纳米颗粒与模型膜之间的相互作用表明,所研究的颗粒之间存在微小差异。本研究的结果表明,观察到的细胞膜损伤是由细胞膜表面的金属释放过程引起的,并强调了 Cu 和 Cu-Zn 金属纳米颗粒与 CuO 纳米颗粒之间的反应性差异。

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