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Surface functionalization of nanoparticles with polyethylene glycol: Effects on protein adsorption and cellular uptake

机译:聚乙二醇对纳米颗粒的表面功能化:对蛋白质吸附和细胞摄取的影响

摘要

Here we have investigated the effect of enshrouding polymer-coated nanoparticles (NPs) with polyethylene glycol (PEG) on the adsorption of proteins and uptake by cultured cells. PEG was covalently linked to the polymer surface to the maximal grafting density achievable under our experimental conditions. Changes in the effective hydrodynamic radius of the NPs upon adsorption of human serum albumin (HSA) and fibrinogen (FIB) were measured in situ using fluorescence correlation spectroscopy. For NPs without a PEG shell, a thickness increase of around 3 nm, corresponding to HSA monolayer adsorption, was measured at high HSA concentration. Only 50% of this value was found for NPs with PEGylated surfaces. While the size increase clearly reveals formation of a protein corona also for PEGylated NPs, fluorescence lifetime measurements and quenching experiments suggest that the adsorbed HSA molecules are buried within the PEG shell. For FIB adsorption onto PEGylated NPs, even less change in NP diameter was observed. In vitro uptake of the NPs by 3T3 fibroblasts was reduced to around 10% upon PEGylation with PEG chains of 10 kDa. Thus, even though the PEG coatings did not completely prevent protein adsorption, the PEGylated NPs still displayed a pronounced reduction of cellular uptake with respect to bare NPs, which is to be expected if the adsorbed proteins are not exposed on the NP surface.
机译:在这里,我们研究了用聚乙二醇(PEG)包裹聚合物包覆的纳米颗粒(NPs)对蛋白质吸附和培养细胞摄取的影响。在我们的实验条件下,PEG共价连接到聚合物表面,以达到最大接枝密度。使用荧光相关光谱法原位测量了吸附人血清白蛋白(HSA)和纤维蛋白原(FIB)后NP的有效流体动力学半径的变化。对于没有PEG壳的NP,在高HSA浓度下测得的厚度增加约3 nm,相当于HSA单层吸附。对于具有聚乙二醇化表面的NP,仅发现该值的50%。尽管尺寸的增加清楚地表明了聚乙二醇化NP也形成了蛋白质电晕,但荧光寿命测量和猝灭实验表明,吸附的HSA分子被掩埋在PEG壳内。对于FIB吸附到PEG化NP上,观察到NP直径的变化更小。当用10 kDa的PEG链进行PEG化时,3T3成纤维细胞对NP的体外吸收降低至约10%。因此,即使PEG涂层不能完全阻止蛋白质的吸附,相对于裸露的NP,PEG化的NP仍显示出明显的细胞摄取减少,如果吸附的蛋白质没有暴露在NP表面上,这是可以预期的。

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