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Cell Chip-Based Monitoring of Toxic Effects of Cosmetic Compounds on Skin Fibroblast Cells

机译:基于细胞芯片的化妆品化合物对皮肤成纤维细胞毒性作用的监测

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The present study estimated the efficacy of electrochemical detection of imidazolidinyl urea-induced cell toxicity in skin human fibroblast cells (HFF cells). The gold nanopunct structures were fabricated through a nanoporous alumina mask, and the structural formations were confirmed via scanning electron microscopy. The HFF cells were allowed to attach to RGD (Arg-Gly-Asp) peptide nanopatterned surfaces, and electrochemical tools were applied to skin cells attached to the chip surface. The HFF cells evidenced inflammation responses to allergens such as imidazolidinyl urea. The cells were subsequently treated with different concentrations of imidazolidinyl urea for 24 h in culture, which induced a change in the cyclic voltammetry (CV) current peak. Treatment with imidazolidinyl urea induced a loss of cell viability and accelerated inflammation in a concentration-dependent manner. The expression level of inflammation-related proteins such as IL-I beta were increased in imidazolidinyl urea-treated cells. The CV results demonstrated that imidazolidinyl urea significantly reduced the current peaks in a dose-dependent manner. The results showed that the current peak was reduced in accordance with the increases in imidazolidinyl urea-induced inflammation. In conclusion, the results of this study suggest that the electrochemical-based chip provides crucial information for improvements to a cell chip system for drug screening applications.
机译:本研究估计了皮肤人成纤维细胞(HFF细胞)中电化学检测咪唑啉基脲诱导的细胞毒性的功效。通过纳米多孔氧化铝掩模制备金纳米点结构,并通过扫描电子显微镜确认结构形成。使HFF细胞附着于RGD(Arg-Gly-Asp)肽纳米图案化的表面,并将电化学工具应用于附着于芯片表面的皮肤细胞。 HFF细胞表现出对过敏原(如咪唑烷基脲)的炎症反应。细胞随后在培养物中用不同浓度的咪唑啉基脲处理24小时,从而引起循环伏安(CV)电流峰值的变化。用咪唑烷基尿素治疗以浓度依赖性方式诱导细胞活力丧失并加速炎症。在咪唑烷基二脲处理的细胞中,炎症相关蛋白(如IL-1β)的表达水平增加。 CV结果表明,咪唑烷基尿素以剂量依赖的方式显着降低了电流峰值。结果表明,电流峰值随咪唑烷基脲引起的炎症增加而降低。总之,这项研究的结果表明,基于电化学的芯片为改进用于药物筛选应用的细胞芯片系统提供了关键信息。

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