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Study on cytotoxicity, cellular uptake and elimination of rare-earth-doped upconversion nanoparticles in human hepatocellular carcinoma cells

机译:人肝细胞癌细胞稀土掺杂稀土掺杂纳米粒子细胞毒性,细胞吸收和消除研究

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The growing use of rare-earth doped upconversion nanoparticles (UCNPs) has caused increasing concern about their biosafety. Here, to understand the toxicity of UCNPs and their mechanism in HepG2 cells, we systematically study the cytotoxicity, uptake and elimination behaviors of three types of UCNPs combined multiple cytotoxicity evaluation means with inductively coupled plasma mass spectrometry (ICP-MS) detection. Sodium yttrium fluoride, doped with 18% (molar ratio) ytterbium and 2% erbium (NaYF4: Yb3+, Er3+) was selected as the model UCNPs with two sizes (35 and 55 nm), and the poly(acrylic acid) and polyethylenimine were selected as the representatives of negative and positive surface coating of UCNPs, respectively. UCNPs were found to induce cytotoxicity in time- and dose-dependent manners, which might be mediated by reactive oxygen species generation and oxidative stress. Apoptosis, inflammation, and metabolic process were enhanced after cells exposed to 200 mg/L UCNPs for 48 h. Increase in the protein levels of cleaved caspased-9, cleaved caspase-3 and Box and decrease in the anti-apoptotic protein, Bcl-2 suggested that the mitochondria mediated pathway was involved in UCNP-induced apoptosis. With the aid of ICP-MS, it demonstrated that the cytotoxicity was associated with internalized amount of UCNPs, which largely relied on their surface properties rather than size in the tested range. By comparing UCNPs with Y3+ ions, it demonstrated that NPs properties played a nonnegligible role in the cytotoxicity of UCNPs. These findings provide new insights for fundamental understanding of cytotoxicity of UCNPs and may contribute to more rational use of these materials in the future.
机译:罕见使用稀土掺杂上转化纳米粒子(UCNP)对其生物安全产生了越来越多的问题。在这里,为了了解UCNP的毒性及其在HepG2细胞中的机制,我们系统地研究了三种UCNPS组合多种细胞毒性评估装置的细胞毒性,摄取和消除行为,具有电感耦合等离子体质谱(ICP-MS)检测。选择氟化钠,掺杂18%(摩尔比)镱和2%erbium(Nayf4:Yb3 +,ER3 +)作为具有两种尺寸(35和55nm)的模型UCNP,以及聚(丙烯酸)和聚乙烯亚胺是选择作为UCNP的阴性和正面涂层的代表。发现UCNPS以时间和剂量依赖的方式诱导细胞毒性,这可能由反应性氧物种产生和氧化应激介导。细胞凋亡,炎症和代谢过程在暴露于200mg / L的Ucnps 48小时后得到增强。增加裂解的半胱氨酸-9的蛋白质水平,切割的caspase-3和盒子和抗凋亡蛋白的减少,Bcl-2表明线粒体介导的途径参与了UCNP诱导的细胞凋亡。借助ICP-MS的借助,证明细胞毒性与内化量的UCNP相关,其在很大程度上依赖于其表面性质而不是测试范围内的大小。通过将UCNP与Y3 +离子进行比较,证明NPS属性在UCNP的细胞毒性中发挥了非阻毒性作用。这些调查结果为UCNP的细胞毒性的基本理解提供了新的见解,并可能有助于将来更合理地使用这些材料。

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