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通过与分子大小可比的合成纳米孔直接可视化单分子易位。

Direct visualization of single-molecule translocations through synthetic nanopores comparable in size to a molecule.

机构信息

Departments of Electrical Engineering and Biological Science, University of Notre Dame, Notre Dame, Indiana 46556, United States.

出版信息

ACS Nano. 2013 May 28;7(5):4057-69. doi: 10.1021/nn400182s. Epub 2013 May 1.

DOI:10.1021/nn400182s
PMID:23607372
Abstract

A nanopore is the ultimate analytical tool. It can be used to detect DNA, RNA, oligonucleotides, and proteins with submolecular sensitivity. This extreme sensitivity is derived from the electric signal associated with the occlusion that develops during the translocation of the analyte across a membrane through a pore immersed in electrolyte. A larger occluded volume results in an improvement in the signal-to-noise ratio, and so the pore geometry should be made comparable to the size of the target molecule. However, the pore geometry also affects the electric field, the charge density, the electro-osmotic flow, the capture volume, and the response time. Seeking an optimal pore geometry, we tracked the molecular motion in three dimensions with high resolution, visualizing with confocal microscopy the fluorescence associated with DNA translocating through nanopores with diameters comparable to the double helix, while simultaneously measuring the pore current. Measurements reveal single molecules translocating across the membrane through the pore commensurate with the observation of a current blockade. To explain the motion of the molecule near the pore, finite-element simulations were employed that account for diffusion, electrophoresis, and the electro-osmotic flow. According to this analysis, detection using a nanopore comparable in diameter to the double helix represents a compromise between sensitivity, capture volume, the minimum detectable concentration, and response time.

摘要

纳米孔是终极分析工具。它可以用于检测 DNA、RNA、寡核苷酸和蛋白质,具有亚分子灵敏度。这种极端灵敏度源于与阻塞相关的电信号,阻塞是在分析物通过浸入电解质中的孔穿过膜迁移时产生的。更大的阻塞体积可提高信噪比,因此孔几何形状应与目标分子的大小相媲美。然而,孔几何形状也会影响电场、电荷密度、电动流、捕获体积和响应时间。为了寻求最佳的孔几何形状,我们以高分辨率跟踪分子在三维空间中的运动,通过共焦显微镜可视化与 DNA 通过与双螺旋相当的直径的纳米孔迁移相关的荧光,同时测量孔电流。测量结果显示,单个分子穿过膜穿过与电流阻断观察一致的孔迁移。为了解释分子在孔附近的运动,采用了考虑扩散、电泳和电动流的有限元模拟。根据该分析,使用直径与双螺旋相当的纳米孔进行检测是在灵敏度、捕获体积、最小可检测浓度和响应时间之间的折衷。

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Direct visualization of single-molecule translocations through synthetic nanopores comparable in size to a molecule.通过与分子大小可比的合成纳米孔直接可视化单分子易位。
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