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Elucidating the mechanism of the surface functionalization dependent neurotoxicity of graphene family nanomaterials

机译:阐明表面的机制功能化的依赖的神经毒性石墨烯纳米材料家族

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摘要

Graphene family nanomaterials (GFNs) have shown great potential for biological and environmental applications; however, their future use has been debated due to their reported potential neurotoxicity. Moreover, the effects of surface functionalization on their biological end points are largely unknown. Here, we compared the effects of reduced graphene oxide (RGO), and carboxylated (G-COOH), hydroxylated (G-OH) and aminated (G-NH2) graphene nanosheets on human neuroblastoma cells (SK-N-SH). All GFNs inhibited cellular growth at concentrations of 0.1-10 mg L(-1)after 24 h exposure. The toxicity was attenuated over longer exposure times, with the exception of G-NH2. Although the overall acute toxicity followed the order: G-OH approximate to G-COOH > RGO > G-NH2, G-NH(2)induced more persistent toxicity and more metabolic disturbance compared to the other GFNs, with lipid and carbohydrate metabolism being the most affected. The potential for physical disruption of the lipid membrane and oxidative damage induced by GFNs varied with different functionalization, which accounts for the observed differences in neurotoxicity. This study provides significant insights into the neurological effects of GFNs, and suggests that G-NH(2)is not as safe as reported in many previous studies. The neurological effect of GFNs over longer term exposure should be considered in future studies.
机译:石墨烯纳米材料家族(GFNs)显示生物和环境潜力巨大应用程序;讨论由于其报道的潜力神经毒性。功能化生物结束点在很大程度上是未知的。减少了氧化石墨烯的影响(RGO),羧酸盐(G-COOH),羟化(G-OH)和胺化了的(G-NH2)石墨烯nanosheets人类神经母细胞瘤细胞(SK-N-SH)。细胞浓度增长0.1 -10毫克L (1) 24 h后曝光。减毒在长时间曝光,G-NH2除外。毒性的秩序:G-OH近似持久性毒性和更多的代谢干扰其他GFNs相比,脂类和碳水化合物代谢受到影响。脂质膜和氧化损伤GFNs引起的不同而不同功能化,占观察神经毒性的差异。提供了重要的见解神经的影响GFNs,表明G-NH(2)没有安全的报道很多先前的研究。在长期接触应该考虑未来的研究。

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