首页> 外文期刊>Annals of Occupational Hygiene >Cytotoxicity and Genotoxicity of Nanosized and Microsized Titanium Dioxide and Iron Oxide Particles in Syrian Hamster Embryo Cells
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Cytotoxicity and Genotoxicity of Nanosized and Microsized Titanium Dioxide and Iron Oxide Particles in Syrian Hamster Embryo Cells

机译:纳米和超细二氧化钛和氧化铁颗粒在叙利亚仓鼠胚胎细胞中的细胞毒性和遗传毒性

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Potential differences in the toxicological properties of nanosized and non-nanosized particles have been notably pointed out for titanium dioxide (TiO2) particles, which are currently widely produced and used in many industrial areas. Nanoparticles of the iron oxides magnetite (Fe3O4) and hematite (Fe2O3) also have many industrial applications but their toxicological properties are less documented than those of TiO2. In the present study, the in vitro cytotoxicity and genotoxicity of commercially available nanosized and microsized anatase TiO2, rutile TiO2, Fe3O4, and Fe2O3 particles were compared in Syrian hamster embryo (SHE) cells. Samples were characterized for chemical composition, primary particle size, crystal phase, shape, and specific surface area. In acellular assays, TiO2 and iron oxide particles were able to generate reactive oxygen species (ROS). At the same mass dose, all nanoparticles produced higher levels of ROS than their microsized counterparts. Measurement of particle size in the SHE culture medium showed that primary nanoparticles and microparticles are present in the form of micrometric agglomerates of highly poly-dispersed size. Uptake of primary particles and agglomerates by SHE exposed for 24 h was observed for all samples. TiO2 samples were found to be more cytotoxic than iron oxide samples. Concerning primary size effects, anatase TiO2, rutile TiO2, and Fe2O3 nanoparticles induced higher cytotoxicity than their microsized counterparts after 72 h of exposure. Over this treatment time, anatase TiO2 and Fe2O3 nanoparticles also produced more intracellular ROS compared to the microsized particles. However, similar levels of DNA damage were observed in the comet assay after 24 h of exposure to anatase nanoparticles and microparticles. Rutile microparticles were found to induce more DNA damage than the nanosized particles. However, no significant increase in DNA damage was detected from nanosized and microsized iron oxides. None of the samples tested showed significant induction of micronuclei formation after 24 h of exposure. In agreement with previous size-comparison studies, we suggest that in vitro cytotoxicity and genotoxicity induced by metal oxide nanoparticles are not always higher than those induced by their bulk counterparts.
机译:对于二氧化钛(TiO 2 )颗粒,目前已经指出了纳米级和非纳米级颗粒在毒理学性质上的潜在差异,而二氧化钛颗粒目前在许多工业领域得到广泛使用。氧化铁磁铁矿(Fe 3 O 4 )和赤铁矿(Fe 2 O 3 )的纳米颗粒也具有在工业上有许多应用,但其毒理学特性却比TiO 2 少。在本研究中,市售的纳米和微米锐钛矿型TiO 2 ,金红石型TiO 2 ,Fe 3 O <的体外细胞毒性和遗传毒性在叙利亚仓鼠胚胎(SHE)细胞中比较了sub> 4 和Fe 2 O 3 颗粒。对样品的化学成分,一次粒径,晶相,形状和比表面积进行表征。在脱细胞分析中,TiO 2 和氧化铁颗粒能够产生活性氧(ROS)。在相同的质量剂量下,所有纳米粒子产生的R​​OS水平均高于其微米级对应物。 SHE培养基中粒径的测量表明,初级纳米颗粒和微粒以高度多分散尺寸的微米级附聚物的形式存在。对于所有样品,观察到暴露于SHE的24小时都吸收了初级颗粒和团聚体。发现TiO 2 样品比氧化铁样品更具细胞毒性。关于初级尺寸效应,锐钛矿型TiO 2 ,金红石型TiO 2 和Fe 2 O 3 纳米颗粒诱导更高的细胞毒性暴露72小时后,它们的体积比同尺寸的同类产品要小。在此处理时间内,与超微粒相比,锐钛矿型TiO 2 和Fe 2 O 3 纳米颗粒还产生更多的细胞内ROS。但是,暴露于锐钛矿纳米颗粒和微粒24小时后,在彗星试验中观察到了相似程度的DNA损伤。发现金红石微粒比纳米微粒引起更多的DNA损伤。然而,从纳米和微米尺寸的氧化铁中未检测到DNA损伤的显着增加。暴露24小时后,所有测试样品均未显示出明显诱导的微核形成。与先前的尺寸比较研究一致,我们建议金属氧化物纳米颗粒诱导的体外细胞毒性和遗传毒性并不总是高于其体积对应物诱导的。

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