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银纳米粒子(AgNPs)对多棘游仆虫模型的毒性:激活的分子机制与剂量和颗粒大小有关。

Toxicity of silver nanoparticles (AgNPs) in the model ciliate Paramecium multimicronucleatum: Molecular mechanisms of activation are dose- and particle size-dependent.

机构信息

The Fujian Provincial Key Laboratory for Coastal Ecology and Environmental Studies, College of the Environment and Ecology, Xiamen University, Xiamen 361005, Fujian, China; Guangzhou Key Laboratory of Subtropical Biodiversity and Biomonitoring, South China Normal University, Guangzhou 510631, China.

Guangzhou Key Laboratory of Subtropical Biodiversity and Biomonitoring, South China Normal University, Guangzhou 510631, China.

出版信息

Eur J Protistol. 2021 Oct;81:125792. doi: 10.1016/j.ejop.2021.125792. Epub 2021 Apr 8.

Abstract

Current understanding of toxicity mechanisms of nanoparticles is still far from comprehensive, partly because of the neglect of control factors such as the dependence of mechanism activation on the exposure dosage and particle size. To reveal molecular mechanisms of silver nanoparticle (AgNP) toxicity, the model ciliate Paramecium multimicronucleatum was exposed for 12 h to different concentrations of AgNPs with particle size of 20 nm (0.08, 0.12, and 0.30 mg/l) and 40 nm (0.08 and 0.30 mg/l). Transcriptomes of the tested ciliates were then analyzed based on dendrograms of gene expression, Gene Ontology (GO) terms, KEGG (Kyoto Encyclopedia of Genes and Genomes) pathways, and up- and down-regulated genes. Results showed that: (1) toxicity mechanisms of AgNP revealed by analyses of GO and KEEG were significantly involved in the metabolic pathways of nutrients and the biosynthesis of macromolecules; (2) the top five up-regulated genes were mainly related to biological oxidation, biosynthesis, and oxidative stress, while top five down-regulated genes were mainly related to glycolysis; (3) activated mechanisms varied both in quantity and in type with dosages and particle sizes of AgNPs; (4) AgNP-treatments with different exposure dosages and particle sizes can produce the same toxicity in terms of 12 h-EC, but the underlying molecular mechanisms differed significantly. In brief, this study provides insights into the molecular mechanisms of AgNP toxicity through transcriptome analyses and confirmed their dependence of activation on the exposure dosage and particle size of AgNPs.

摘要

目前,人们对纳米颗粒毒性机制的理解还远远不够全面,部分原因是忽视了控制因素,如机制激活对暴露剂量和颗粒尺寸的依赖性。为了揭示银纳米颗粒(AgNP)毒性的分子机制,我们用粒径为 20nm(0.08、0.12 和 0.30mg/L)和 40nm(0.08 和 0.30mg/L)的 AgNP 处理多小核草履虫 12 小时,然后根据基因表达的系统发育树、基因本体论(GO)术语、京都基因与基因组百科全书(KEGG)途径以及上调和下调基因对测试纤毛虫的转录组进行了分析。结果表明:(1)GO 和 KEEG 分析揭示的 AgNP 毒性机制显著参与了营养物质的代谢途径和生物大分子的生物合成;(2)前五个上调基因主要与生物氧化、生物合成和氧化应激有关,而前五个下调基因主要与糖酵解有关;(3)激活机制在数量和类型上都随 AgNP 的剂量和粒径而变化;(4)不同暴露剂量和粒径的 AgNP 处理在 12 小时 EC 方面可能产生相同的毒性,但潜在的分子机制有很大的不同。总之,本研究通过转录组分析深入了解了 AgNP 毒性的分子机制,并证实了其激活机制依赖于 AgNP 的暴露剂量和粒径。

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