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表征纳米颗粒在片上集成黑脂膜上的侧向摩擦力。

Characterizing the lateral friction of nanoparticles on on-chip integrated black lipid membranes.

机构信息

Department of Chemistry and the Photonics Center, Boston University, Boston, MA 02215, USA.

出版信息

Small. 2013 Mar 25;9(6):876-84. doi: 10.1002/smll.201202005. Epub 2012 Nov 23.

Abstract

The use of nanoparticles (NPs) in biomedical applications creates a need for appropriate model systems to systematically investigate NP-membrane interactions under well-defined conditions. Black lipid membranes (BLMs) are free-floating membranes with defined composition that are ideally suited for characterizing NP-membrane interactions free of any potential perturbation through a supporting substrate. Herein, arrays of microfabricated BLMs are integrated into a chip-based platform that is compatible with high-speed optical NP tracking. This system is used to investigate the lateral diffusion of 40 nm gold spheres tethered to biotinylated lipids through antibody-functionalized ligands (single-stranded DNA or polyethylene glycol). Although the NPs show an almost free and ergodic diffusion, their lateral motion is subject to substantial drag at the membrane surface, which leads to systematically smaller diffusion coefficients than those obtained for lipids in the membrane through fluorescence recovery after photobleaching. The lateral mobility of the NPs is influenced by the chemical composition and salt concentration at the NP-membrane interface, but is independent of the ligand density in the membrane. Together with the observation that nanoprisms, which have a larger relative contact area with the membrane than spherical NPs, show an even slower diffusion, these findings indicate that the lateral mobility of NPs tethered in close vicinity to a membrane is significantly reduced by the friction at the NP-membrane interface.

摘要

纳米粒子(NPs)在生物医学应用中的使用需要适当的模型系统,以便在明确定义的条件下系统地研究 NP-膜相互作用。黑脂膜(BLM)是具有定义组成的自由浮动膜,非常适合在没有任何潜在干扰的情况下,通过支撑基底来表征 NP-膜相互作用。本文将微加工的 BLM 阵列集成到一种基于芯片的平台中,该平台与高速光学 NP 跟踪兼容。该系统用于研究通过抗体功能化配体(单链 DNA 或聚乙二醇)固定在生物素化脂质上的 40nm 金球的横向扩散。尽管 NPs 表现出几乎自由和遍历的扩散,但它们的横向运动在膜表面受到很大的阻力,导致扩散系数比通过光漂白后荧光恢复测量的膜中脂质的扩散系数小得多。NP 的横向迁移受 NP-膜界面处的化学组成和盐浓度的影响,但不受膜中配体密度的影响。与观察到的纳米棱柱体相比,纳米棱柱体与膜的相对接触面积更大,扩散速度更慢,这些发现表明,与膜紧密结合的 NP 的横向迁移能力由于 NP-膜界面处的摩擦而大大降低。

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