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Polymorph- and size-dependent uptake and toxicity of TiO_2 nanoparticles in living lung epithelial cells

机译:活肺上皮细胞中TiO_2纳米粒子的多晶型和尺寸依赖性摄取和毒性

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The cellular uptake and distribution of five types of well-characterized anatase and rutile TiO_2 nanoparticles (NPs) in A549 lung epithelial cells is reported. Static light scattering (SLS), in-vitro Raman microspectroscopy (μ-Raman) and transmission electron spectroscopy (TEM) reveal an intimate correlation between the intrinsic physicochemical properties of the NPs, particle agglomeration, and cellular NP uptake. It is shown that μ-Raman facilitates chemical-, polymorph-, and size-specific discrimination of endosomal-particle cell uptake and the retention of particles in the vicinity of organelles, including the cell nucleus, which quantitatively correlates with TEM and SLS data. Depth-profiling μ-Raman coupled with hyperspectral data analysis confirms the location of the NPs in the cells and shows that the NPs induce modifications of the biological matrix. NP uptake is found to be kinetically activated and strongly dependent on the hard agglomeration sizeanot the primary particle sizeawhich quantitatively agrees with the measured intracellular oxidative stress. Pro-inflammatory responses are also found to be sensitive to primary particle size.
机译:报道了在A549肺上皮细胞中五种特征充分的锐钛矿和金红石型TiO_2纳米颗粒(NPs)的细胞吸收和分布。静态光散射(SLS),体外拉曼光谱(μ-Raman)和透射电子光谱(TEM)揭示了NP的内在物理化学性质,颗粒团聚和细胞NP吸收之间的密切关系。结果表明,μ-拉曼促进了内体颗粒细胞摄取的化学,多态性和大小特异性判别,以及颗粒在细胞器附近(包括细胞核)的保留,这与TEM和SLS数据定量相关。深度分析μ拉曼结合高光谱数据分析证实了NP在细胞中的位置,并表明NP诱导了生物基质的修饰。发现NP吸收是动力学激活的,并且强烈依赖于硬团聚尺寸而不是初级颗粒尺寸a,初级颗粒尺寸在数量上与所测量的细胞内氧化应激一致。还发现促炎反应对初级粒径敏感。

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