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利用纳米多孔金电极进行电引导的DNA固定和多重DNA检测。

Electrically Guided DNA Immobilization and Multiplexed DNA Detection with Nanoporous Gold Electrodes.

作者信息

Veselinovic Jovana, Li Zidong, Daggumati Pallavi, Seker Erkin

机构信息

Department of Chemical Engineering, University of California-Davis, Davis, CA 95616, USA.

Department of Biomedical Engineering, University of California-Davis, Davis, CA 95616, USA.

出版信息

Nanomaterials (Basel). 2018 May 21;8(5):351. doi: 10.3390/nano8050351.

Abstract

Molecular diagnostics have significantly advanced the early detection of diseases, where the electrochemical sensing of biomarkers (e.g., DNA, RNA, proteins) using multiple electrode arrays (MEAs) has shown considerable promise. Nanostructuring the electrode surface results in higher surface coverage of capture probes and more favorable orientation, as well as transport phenomena unique to nanoscale, ultimately leading to enhanced sensor performance. The central goal of this study is to investigate the influence of electrode nanostructure on electrically-guided immobilization of DNA probes for nucleic acid detection in a multiplexed format. To that end, we used nanoporous gold (np-Au) electrodes that reduced the limit of detection (LOD) for DNA targets by two orders of magnitude compared to their planar counterparts, where the LOD was further improved by an additional order of magnitude after reducing the electrode diameter. The reduced electrode diameter also made it possible to create a np-Au MEA encapsulated in a microfluidic channel. The electro-grafting reduced the necessary incubation time to immobilize DNA probes into the porous electrodes down to 10 min (25-fold reduction compared to passive immobilization) and allowed for grafting a different DNA probe sequence onto each electrode in the array. The resulting platform was successfully used for the multiplexed detection of three different biomarker genes relevant to breast cancer diagnosis.

摘要

分子诊断技术显著推动了疾病的早期检测,其中利用多电极阵列(MEA)对生物标志物(如DNA、RNA、蛋白质)进行电化学传感已展现出巨大潜力。对电极表面进行纳米结构化处理可实现捕获探针更高的表面覆盖率和更有利的取向,以及纳米尺度特有的传输现象,最终提升传感器性能。本研究的核心目标是探究电极纳米结构对以多重形式进行核酸检测时DNA探针电引导固定的影响。为此,我们使用了纳米多孔金(np-Au)电极,与平面电极相比,其将DNA靶标的检测限(LOD)降低了两个数量级,在减小电极直径后,LOD又进一步提高了一个数量级。减小电极直径还使得制造封装在微流控通道中的np-Au MEA成为可能。电接枝将把DNA探针固定到多孔电极所需的孵育时间缩短至10分钟(与被动固定相比减少了25倍),并允许在阵列中的每个电极上接枝不同的DNA探针序列。所得平台成功用于与乳腺癌诊断相关的三种不同生物标志物基因的多重检测。

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