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Effects of flame made zinc oxide particles in human lung cells - a comparison of aerosol and suspension exposures

机译:火焰制成的氧化锌颗粒在人肺细胞中的作用-气溶胶和悬浮液暴露的比较

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Background Predominantly, studies of nanoparticle ( NPs ) toxicology in vitro are based upon the exposure of submerged cell cultures to particle suspensions. Such an approach however, does not reflect particle inhalation. As a more realistic simulation of such a scenario, efforts were made towards direct delivery of aerosols to air-liquid-interface cultivated cell cultures by the use of aerosol exposure systems. This study aims to provide a direct comparison of the effects of zinc oxide (ZnO) NPs when delivered as either an aerosol, or in suspension to a triple cell co-culture model of the epithelial airway barrier. To ensure dose–equivalence, ZnO-deposition was determined in each exposure scenario by atomic absorption spectroscopy. Biological endpoints being investigated after 4 or 24h incubation include cytotoxicity, total reduced glutathione, induction of antioxidative genes such as heme-oxygenase 1 (HO–1) as well as the release of the (pro)-inflammatory cytokine TNFα. Results Off-gases released as by-product of flame ZnO synthesis caused a significant decrease of total reduced GSH and induced further the release of the cytokine TNFα, demonstrating the influence of the gas phase on aerosol toxicology. No direct effects could be attributed to ZnO particles. By performing suspension exposure to avoid the factor “flame-gases”, particle specific effects become apparent. Other parameters such as LDH and HO–1 were not influenced by gaseous compounds: Following aerosol exposure, LDH levels appeared elevated at both timepoints and the HO–1 transcript correlated positively with deposited ZnO-dose. Under submerged conditions, the HO–1 induction scheme deviated for 4 and 24h and increased extracellular LDH was found following 24h exposure. Conclusion In the current study, aerosol and suspension-exposure has been compared by exposing cell cultures to equivalent amounts of ZnO. Both exposure strategies differ fundamentally in their dose–response pattern. Additional differences can be found for the factor time: In the aerosol scenario, parameters tend to their maximum already after 4h of exposure, whereas under submerged conditions, effects appear most pronounced mainly after 24h. Aerosol exposure provides information about the synergistic interplay of gaseous and particulate phase of an aerosol in the context of inhalation toxicology. Exposure to suspensions represents a valuable complementary method and allows investigations on particle-associated toxicity by excluding all gas–derived effects.
机译:背景技术主要地,体外纳米颗粒(NP)毒理学研究基于浸没细胞培养物暴露于颗粒悬浮液。但是,这种方法不能反映颗粒的吸入。作为这种情况的更现实的模拟,已努力通过使用气溶胶暴露系统将气溶胶直接递送到气液界面培养的细胞培养物中。这项研究旨在提供直接比较,以气雾剂形式或以悬浮液形式输送至上皮气道屏障的三细胞共培养模型时,氧化锌(ZnO)NP的作用。为了确保剂量相等,通过原子吸收光谱法确定每种暴露情况下的ZnO沉积量。孵育4或24小时后要研究的生物学终点包括细胞毒性,谷胱甘肽总量减少,抗氧化基因(如血红素加氧酶1(HO-1))的诱导以及(促)炎性细胞因子TNFα的释放。结果火焰状ZnO合成的副产物释放的废气导致总还原GSH的显着降低,并进一步诱导了细胞因子TNFα的释放,证明了气相对气溶胶毒理学的影响。没有直接影响可归因于ZnO颗粒。通过进行悬浮液暴露以避免“火焰气体”因素,颗粒特有的效果变得显而易见。其他参数,例如LDH和HO-1不受气态化合物的影响:气溶胶暴露后,LDH水平在两个时间点均升高,HO-1转录本与ZnO剂量呈正相关。在淹没条件下,HO-1诱导方案在4和24h时发生偏离,暴露24h后发现细胞外LDH增加。结论在当前的研究中,通过将细胞培养物暴露于等量的ZnO中来比较气溶胶和悬浮液暴露。两种接触策略的剂量反应模式都有根本不同。在时间因素上还可以发现其他差异:在气雾剂情况下,参数在暴露4小时后已趋于最大,而在浸没条件下,效果主要在24小时后显现出来。在吸入毒理学方面,暴露于气溶胶​​可提供有关气溶胶的气态和颗粒相协同相互作用的信息。接触悬浮液是一种有价值的补充方法,可以排除所有气体衍生的影响,从而研究与颗粒相关的毒性。

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