In vitro comparative cytotoxicity study of aminated polystyrene, zinc oxide and silver nanoparticles on a cervical cancer cell line.

IF 1.9 4区 医学 Q3 CHEMISTRY, MULTIDISCIPLINARY Drug and Chemical Toxicology Pub Date : 2019-01-01 Epub Date: 2018-01-23 DOI:10.1080/01480545.2018.1424181
Akash Sharma, Brian Gorey, Alan Casey
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引用次数: 18

Abstract

Nanoparticles use in nano-biotechnology applications have increased significantly with Aminated polystyrene amine (AmPs NP), Zinc oxide (ZnO NP), and Silver (Ag NP) nanoparticles utilized in wide variety of consumer products. This has presented a number of concerns due to their increased exposure risks and associated toxicity on living systems. Changes in the structural and physicochemical properties of nanoparticles can lead to changes in biological activities. This study investigates, compares, and contrasts the potential toxicity of AmPs, ZnO and Ag NPs on an in vitro model (HeLa cells) and assesses the associated mechanism for their corresponding cytotoxicity relative to the surface material. It was noted that NPs exposure attributed to the reduction in cell viability and high-level induction of oxidative stress. All three test particles were noted to induce ROS to varying degrees which is irrespective of the attached surface group. Cell cycle analysis indicated a G2/M phase cell arrest, with the corresponding reduction in G0/G1 and S phase cells resulting in caspase-mediated apoptotic cell death. These findings suggest that all three NPs resulted in the decrease in cell viability, increase intracellular ROS production, induce cell cycle arrest at the G2/M phase and finally result in cell death by caspase-mediated apoptosis, which is irrespective of their differences in physiochemical properties and attached surface groups.

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胺化聚苯乙烯、氧化锌和纳米银对宫颈癌细胞系的体外细胞毒性比较研究。
纳米粒子在纳米生物技术中的应用随着胺化聚苯乙烯胺(AmPs NP)、氧化锌(ZnO NP)和银(Ag NP)纳米粒子在各种消费产品中的应用而显著增加。由于其暴露风险增加以及对生命系统的相关毒性,这引起了许多关注。纳米颗粒的结构和物理化学性质的变化可以导致生物活性的变化。本研究对AmPs、ZnO和Ag NPs在体外模型(HeLa细胞)上的潜在毒性进行了研究、比较和对比,并评估了它们相对于表面材料的相应细胞毒性的相关机制。研究指出,NPs暴露可归因于细胞活力降低和氧化应激的高水平诱导。所有三种测试颗粒都注意到不同程度的诱导ROS,这与附着的表面基团无关。细胞周期分析显示G2/M期细胞阻滞,G0/G1和S期细胞相应减少,导致caspase介导的凋亡细胞死亡。这些发现表明,这三种NPs都导致细胞活力降低,细胞内ROS产生增加,诱导细胞周期阻滞在G2/M期,最终通过caspase介导的凋亡导致细胞死亡,而这与它们的理化性质和附着表面基团的差异无关。
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来源期刊
Drug and Chemical Toxicology
Drug and Chemical Toxicology 医学-毒理学
CiteScore
6.00
自引率
3.80%
发文量
99
审稿时长
3 months
期刊介绍: Drug and Chemical Toxicology publishes full-length research papers, review articles and short communications that encompass a broad spectrum of toxicological data surrounding risk assessment and harmful exposure. Manuscripts are considered according to their relevance to the journal. Topics include both descriptive and mechanics research that illustrates the risk assessment implications of exposure to toxic agents. Examples of suitable topics include toxicological studies, which are structural examinations on the effects of dose, metabolism, and statistical or mechanism-based approaches to risk assessment. New findings and methods, along with safety evaluations, are also acceptable. Special issues may be reserved to publish symposium summaries, reviews in toxicology, and overviews of the practical interpretation and application of toxicological data.
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