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Intracellular accumulation of indium ions released from nanoparticles induces oxidative stress proinflammatory response and DNA damage

机译:从纳米粒子释放的铟离子在细胞内的积累会诱导氧化应激促炎反应和DNA损伤

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摘要

Due to the widespread use of indium tin oxide (ITO), it is important to investigate its effect on human health. In this study, we evaluated the cellular effects of ITO nanoparticles (NPs), indium chloride (InCl3) and tin chloride (SnCl3) using human lung epithelial A549 cells. Transmission electron microscopy and inductively coupled plasma mass spectrometry were employed to study cellular ITO NP uptake. Interestingly, greater uptake of ITO NPs was observed, as compared with soluble salts. ITO NP species released could be divided into two types: ‘indium release ITO’ or ‘tin release ITO’. We incubated A549 cells with indium release ITO, tin release ITO, InCl3 or SnCl2 and investigated oxidative stress, proinflammatory response, cytotoxicity and DNA damage. We found that intracellular reactive oxygen species were increased in cells incubated with indium release ITO, but not tin release ITO, InCl3 or SnCl2. Messenger RNA and protein levels of the inflammatory marker, interleukin-8, also increased following exposure to indium release ITO. Furthermore, the alkaline comet assay revealed that intracellular accumulation of indium ions induced DNA damage. Our results demonstrate that the accumulation of ionic indium, but not ionic tin, from ITO NPs in the intracellular matrix has extensive cellular effects.
机译:由于铟锡氧化物(ITO)的广泛使用,因此研究其对人体健康的影响非常重要。在这项研究中,我们评估了使用人肺上皮A549细胞对ITO纳米颗粒(NPs),氯化铟(InCl3)和氯化锡(SnCl3)的细胞作用。透射电子显微镜和电感耦合等离子体质谱法用于研究细胞对ITO NP的吸收。有趣的是,与可溶性盐相比,可观察到更大的ITO NP吸收。释放的ITO NP种类可分为两种:“铟释放ITO”或“锡释放ITO”。我们将A549细胞与铟释放ITO,锡释放ITO,InCl3或SnCl2进行了孵育,并研究了氧化应激,促炎反应,细胞毒性和DNA损伤。我们发现,与铟释放ITO孵育的细胞中细胞内活性氧种类增加,但与锡释放ITO,InCl3或SnCl2孵育的细胞中没有。暴露于铟释放ITO后,炎症标记物白细胞介素8的信使RNA和蛋白质水平也增加。此外,碱性彗星试验揭示了铟离子在细胞内的积累会诱导DNA损伤。我们的结果表明,细胞内基质中ITO NP中离子性铟(而非离子性锡)的积累具有广泛的细胞效应。

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