金纳米颗粒与常见人体血液蛋白的相互作用。

Interaction of gold nanoparticles with common human blood proteins.

机构信息

Center for Biological Evaluation and Research, Food and Drug Administration, Bethesda, Maryland 20892, USA.

出版信息

ACS Nano. 2010 Jan 26;4(1):365-79. doi: 10.1021/nn9011187.

Abstract

In order to better understand the physical basis of the biological activity of nanoparticles (NPs) in nanomedicine applications and under conditions of environmental exposure, we performed an array of photophysical measurements to quantify the interaction of model gold NPs having a wide range of NP diameters with common blood proteins. In particular, absorbance, fluorescence quenching, circular dichroism, dynamic light scattering, and electron microscopy measurements were performed on surface-functionalized water-soluble gold NPs having a diameter range from 5 to 100 nm in the presence of common human blood proteins: albumin, fibrinogen, gamma-globulin, histone, and insulin. We find that the gold NPs strongly associate with these essential blood proteins where the binding constant, K, as well as the degree of cooperativity of particle--protein binding (Hill constant, n), depends on particle size and the native protein structure. We also find tentative evidence that the model proteins undergo conformational change upon association with the NPs and that the thickness of the adsorbed protein layer (bare NP diameter <50 nm) progressively increases with NP size, effects that have potential general importance for understanding NP aggregation in biological media and the interaction of NP with biological materials broadly.

摘要

为了更好地理解纳米医学应用中纳米颗粒 (NPs) 的生物学活性的物理基础和在环境暴露条件下的情况,我们进行了一系列光物理测量,以量化具有广泛粒径范围的模型金 NPs 与常见血液蛋白质之间的相互作用。特别是,在存在常见的人类血液蛋白质(白蛋白、纤维蛋白原、γ-球蛋白、组蛋白和胰岛素)的情况下,对具有 5 至 100nm 直径范围的表面功能化水溶性金 NPs 进行了吸收、荧光猝灭、圆二色性、动态光散射和电子显微镜测量。我们发现金 NPs 与这些基本血液蛋白质强烈结合,其中结合常数 K 以及颗粒-蛋白质结合的协同度 (Hill 常数 n) 取决于颗粒尺寸和天然蛋白质结构。我们还发现了初步证据表明,模型蛋白质在与 NPs 结合时会发生构象变化,并且吸附蛋白质层的厚度(裸 NP 直径 <50nm)随 NP 尺寸的增加而逐渐增加,这些效应对于理解 NP 在生物介质中的聚集以及 NP 与广泛的生物材料的相互作用具有普遍重要意义。

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