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Relating the composition and interface interactions in the hard corona of gold nanoparticles to the induced response mechanisms in living cells

机译:相关的组成和接口交互困难电晕的黄金纳米颗粒诱导反应机制在活细胞

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摘要

Understanding the formation of the intracellular protein corona of nanoparticles is essential for a wide range of bio- and nanomedical applications. The innermost layer of the protein corona, the hard corona, directly interacts with the nanoparticle surface, and by shielding the surface, it has a deterministic effect on the intracellular processing of the nanoparticle. Here, we combine a direct qualitative analysis of the hard corona composition of gold nanoparticles with a detailed structural characterization of the molecules in their interaction with the nanoparticle surface and relate both to the effects they have on the ultrastructure of living cells and the processing of the gold nanoparticles. Cells from the cell lines HCT-116 and A549 were incubated with 30 nm citrate-stabilized gold nanoparticles and with their aggregates in different culture media. The combined results of mass spectrometry based proteomics, cryo soft X-ray nanotomography and surface-enhanced Raman scattering experiments together revealed different uptake mechanisms in the two cell lines and distinct levels of induced cellular stress when incubation conditions were varied. The data indicate that the different incubation conditions lead to changes in the nanoparticle processingviadifferent protein-nanoparticle interfacial interactions. Specifically, they suggest that the protein-nanoparticle surface interactions depend mainly on the surface properties of the gold nanoparticles, that is, the zeta-potential and the resulting changes in the hydrophilicity of the nanoparticle surface, and are largely independent of the cell line, the uptake mechanism and intracellular processing, or the extent of the induced cellular stress.
机译:理解细胞的形成蛋白质电晕的纳米颗粒是至关重要的广泛的生物和纳米医学应用程序。电晕,电晕,直接与之交互纳米颗粒表面,通过屏蔽表面上看,它有决定性的影响细胞内处理的纳米颗粒。在这里,我们的直接定性分析结合起来电晕金纳米粒子的合成详细的结构表征分子的相互作用纳米颗粒表面和联系影响他们对生活的超微结构细胞和黄金的处理纳米粒子。并与30 nm A549被孵化citrate-stabilized金纳米粒子和他们在不同的文化媒体聚合。结合质谱为基础的结果蛋白质组学,低温软x射线nanotomography和表面增强拉曼散射实验显示不同的吸收机制两个细胞系和不同程度的诱导细胞压力当孵化条件多样。孵化条件导致的变化纳米颗粒processingviadifferentprotein-nanoparticle界面交互。具体来说,他们建议protein-nanoparticle表面相互作用取决于主要表面上黄金的属性纳米粒子,即电动电位和结果亲水性的变化纳米颗粒表面,在很大程度上独立的细胞系,吸收机制和细胞内加工,或诱导细胞的压力程度。

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