Toxicology Unit, Applied Biology Division, CSIR - Indian Institute of Chemical Technology, Hyderabad, Telangana, India.
Academy of Scientific and Innovative Research, CSIR - Indian Institute of Chemical Technology, Hyderabad, Telangana, India.
Mutagenesis. 2019 May 29;34(2):181-201. doi: 10.1093/mutage/gey044.
Despite their enormous advantages, nanoparticles (NPs) have elicited disquiet over their safety. Among the numerous NPs, yttrium oxide (Y2O3) NPs are utilised in many applications. However, knowledge about their toxicity is limited, and it is imperative to investigate their potential adverse effects. Therefore, this study explored the effect of 28 days of repeated oral exposure of Wistar rats to 30, 120 and 480 mg/kg body weight (bw) per day of Y2O3 NPs and microparticles (MPs). Before initiation of the study, characterisation of the particles by transmission electron microscopy, dynamic light scattering, Brunauer-Emmett-Teller and laser Doppler velocimetry was undertaken. Genotoxicity was evaluated using the comet and micronucleus (MN) assays. Biochemical markers aspartate transaminase, alanine transaminase, alkaline phosphatase, malondialdehyde, superoxide dismutase, reduced glutathione, catalase and lactate dehydrogenase in serum, liver and kidney were determined. Bioaccumulation of the particles was analysed by inductively coupled plasma optical emission spectrometry. The results of the comet and MN assays showed significant differences between the control and groups treated with 120 and 480 mg/kg bw/day Y2O3 NPs. Significant biochemical alterations were also observed at 120 and 480 mg/kg bw/day. Haematological and histopathological changes were documented. Yttrium (Y) biodistribution was detected in liver, kidney, blood, intestine, lungs, spleen, heart and brain in a dose- and the organ-dependent manner in both the particles. Further, the highest levels of Y were found in the liver and the lowest in the brain of the treated rats. More of the Y from NPs was excreted in the urine than in the faeces. Furthermore, NP-treated rats exhibited much higher absorption and tissue accumulation. These interpretations furnish rudimentary data of the apparent genotoxicity of NPs and MPs of Y2O3 as well as the biodistribution of Y. A no-observed adverse effect level of 30 mg/kg bw/day was found after oral exposure of rats to Y2O3 NPs.
尽管纳米颗粒(NPs)具有巨大的优势,但人们对其安全性仍存在担忧。在众多的 NPs 中,氧化钇(Y2O3)纳米颗粒被应用于许多领域。然而,人们对其毒性的了解有限,因此有必要研究其潜在的不良影响。因此,本研究探讨了 Wistar 大鼠连续口服暴露于 30、120 和 480mg/kg 体重/天的 Y2O3 NPs 和微颗粒(MPs)28 天的影响。在研究开始之前,通过透射电子显微镜、动态光散射、BET 和激光多普勒测速对颗粒进行了特性描述。使用彗星和微核(MN)试验评估遗传毒性。测定血清、肝脏和肾脏中天冬氨酸转氨酶、丙氨酸转氨酶、碱性磷酸酶、丙二醛、超氧化物歧化酶、还原型谷胱甘肽、过氧化氢酶和乳酸脱氢酶等生化标志物。通过电感耦合等离子体光学发射光谱法分析颗粒的生物累积。彗星和 MN 试验的结果表明,对照组与 120 和 480mg/kg bw/day Y2O3 NPs 处理组之间存在显著差异。在 120 和 480mg/kg bw/day 时还观察到了显著的生化变化。还记录了血液学和组织病理学变化。在两种颗粒中,以剂量和器官依赖的方式检测到 Y 在肝脏、肾脏、血液、肠道、肺、脾脏、心脏和大脑中的生物分布。此外,在处理大鼠的肝脏中发现了最高水平的 Y,在大脑中发现了最低水平的 Y。从 NPs 中排泄到尿液中的 Y 比排泄到粪便中的 Y 多。此外,NP 处理的大鼠表现出更高的吸收和组织积累。这些解释提供了 NPs 和 MPs 的 Y2O3 的明显遗传毒性以及 Y 的生物分布的初步数据。大鼠口服暴露于 Y2O3 NPs 后,发现 30mg/kg bw/day 为无观察到不良效应水平。
Zotero 插件