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Nanopore sensing at ultra-low concentrations using single-molecule dielectrophoretic trapping

机译:使用单分子介电电泳技术以超低浓度进行纳米孔传感

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摘要

Single-molecule techniques are being developed with the exciting prospect of revolutionizing the healthcare industry by generating vast amounts of genetic and proteomic data. One exceptionally promising route is in the use of nanopore sensors. However, a well-known complexity is that detection and capture is predominantly diffusion limited. This problem is compounded when taking into account the capture volume of a nanopore, typically 108–1010 times smaller than the sample volume. To rectify this disproportionate ratio, we demonstrate a simple, yet powerful, method based on coupling single-molecule dielectrophoretic trapping to nanopore sensing. We show that DNA can be captured from a controllable, but typically much larger, volume and concentrated at the tip of a metallic nanopore. This enables the detection of single molecules at concentrations as low as 5 fM, which is approximately a 103 reduction in the limit of detection compared with existing methods, while still maintaining efficient throughput.
机译:正在开发单分子技术,其令人激动的前景是通过生成大量的遗传和蛋白质组学数据来彻底改变医疗保健行业。一种非常有前途的途径是使用纳米孔传感器。但是,众所周知的复杂性是检测和捕获主要受扩散限制。考虑到纳米孔的捕获体积(通常比样品体积小10 8 –10 10 倍),这个问题变得更加复杂。为了纠正这种不成比例的问题,我们展示了一种简单而强大的方法,该方法基于将单分子介电电泳与纳米孔传感耦合。我们表明,DNA可以从可控但通常更大的体积中捕获,并集中在金属纳米孔的尖端。这使得能够以低至5 fM的浓度检测单个分子,与现有方法相比,检测限降低了约10 3 ,同时仍保持了有效的通量。

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