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首页> 外文期刊>Journal of toxicology and environmental health, Part A >Differential pulmonary in vitro toxicity of two small-sized polyvinylpyrrolidone-coated silver nanoparticles
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Differential pulmonary in vitro toxicity of two small-sized polyvinylpyrrolidone-coated silver nanoparticles

机译:两种小型聚乙烯吡咯烷酮涂覆银纳米粒子的差异肺体外毒性

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Silver nanoparticles (AgNP), with their important properties, are being used in a range of sectors from industry to medicine, leading to increased human exposure. Hence, their toxicity potential needs to be comprehensively evaluated. It was postulated that within small-sized (<20 nm) polyvinylpyrrolidone-coated silver nanoparticles (PVP-AgNP), minor size differences may significantly induce different toxicity profiles and involve varying cellular pathways. Therefore, the aim of this study was to examine the influence of differing size AgNP with 10 nm (AgNP10) and 20 nm (AgNP20) (up to 100 |jg/ml), as well as to ionic silver as AgNO_3 for 24 and 48 h, using the human lung cell line A549. The effects on cell viability, proliferation, apoptosis, DNA damage and cell cycle dynamics were assessed. Results for both time periods showed that for low concentrations (<5 ng/ml), AgNP20 were more cytotoxic than AgNP10, however, at higher doses, AgNP10 exhibited higher toxicity. For concentrations >50 ug/ml, AgNP10 induced severe DNA damage (comet class 3-4), cell cycle arrest at G_2 phase and late-stage apoptosis, while AgNP20 induced cell cycle arrest at S phase and an increase in the percentage sub-G_1 which did not recover after 48 h, and late-stage apoptosis/necrosis. In longer-term exposures, the greater impairment in colony formation due to AgNP exposure than to silver ion supports that nanotoxicity is not exclusively due to the released ion. Data suggest that toxicity mediated by small AgNP (<20 nm) in lung cells is not only dependent on the level of particle internalization, but also on AgNP size and concentration, which may involve varying pathways as targets.
机译:具有重要性质的银纳米粒子(AGNP)正在从工业到医学的一系列部门中使用,导致人类暴露增加。因此,需要全面评估它们的毒性潜力。假设其中,在小尺寸(<20nm)聚乙烯吡咯烷酮涂覆的银纳米粒子(PVP-AGNP)内,轻微尺寸差异可显着诱导不同的毒性曲线并涉及不同的细胞途径。因此,本研究的目的是检查不同尺寸AgNP与10nm(AgNP10)和20nm(AgNP20)(最多100 | JG / mL)的影响,以及24和48的离子银作为AgNO_3 h,使用人肺细胞系A549。评估了对细胞活力,增殖,凋亡,DNA损伤和细胞周期动态的影响。两个时间段的结果表明,对于低浓度(<5ng / ml),AgNP20比AgNP10更具细胞毒性,然而,在更高的剂量下,AgNP10表现出更高的毒性。对于浓度> 50ug / ml,AGNP10诱导严重的DNA损伤(彗星3-4级),在G_2相和晚期细胞凋亡的细胞周期停滞,而AGNP20诱导的细胞周期停滞在S期并增加百分比子 - 48小时后没有恢复的G_1,晚期凋亡/坏死。在长期暴露中,由于AGNP暴露而不是银离子的菌落形成的更大损伤,所述纳米毒性由于释放的离子而不是仅限于纳米毒性。数据表明,肺细胞中的小AgNP(<20nm)介导的毒性不仅取决于颗粒内化水平,还涉及AgNP尺寸和浓度,这可能涉及不同的途径作为靶标。

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