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适配链的概念验证应用:DNA适配体的配体诱导自组装

A proof of concept application of aptachain: ligand-induced self-assembly of a DNA aptamer.

作者信息

Neves Miguel A D, Slavkovic Sladjana, Reinstein Oren, Shoara Aron A, Johnson Philip E

机构信息

Department of Chemistry & Centre for Research on Biomolecular Interactions, York University 4700 Keele St. Toronto Ontario Canada M3J 1P3

出版信息

RSC Adv. 2019 Jan 14;9(3):1690-1695. doi: 10.1039/c8ra07462c. eCollection 2019 Jan 9.

Abstract

A challenge for the use of aptamers as biosensors is how to signal the occurrence of their ligand binding event into a signal that can be exploited in a detection scheme. Here, we present the concept of "aptachain" formation, where an aptamer is split into two overlapping or staggered strands and assembles into an extended oligomer upon ligand binding. This assembly of aptamers can then be used as a way to detect ligand binding by the aptamer. As an example of this concept, we employed the cocaine-binding aptamer as a model system, used its ability to tightly bind quinine and demonstrated its capability in a gold nanoparticle-based biosensing application. We used isothermal titration calorimetry to demonstrate that, when split into two overlapping DNA strands, the aptamer remains functional. Size-exclusion chromatography showed that the quinine-bound oligos form a larger assembly of aptamer units than in the absence of ligand. Finally, we used the oligomer forming ability of the aptachain oligos in a biosensor application for quinine that brings gold nanoparticles closer together resulting in a shift in their plasmonic resonance to a longer wavelength and an observed colour shift. We propose that splitting aptamers into overlapping strands that form oligomers in the presence of a ligand, aptachain formation, will be generally applicable to aptamers and prove useful in a variety of biotechnology applications.

摘要

将适体用作生物传感器面临的一个挑战是如何将其配体结合事件的发生转化为可在检测方案中利用的信号。在此,我们提出了“适体链”形成的概念,即将一个适体拆分成两条重叠或交错的链,并在配体结合时组装成一个延伸的寡聚物。然后,这种适体的组装可作为检测适体配体结合的一种方法。作为这一概念的一个例子,我们以可卡因结合适体为模型系统,利用其紧密结合奎宁的能力,并在基于金纳米颗粒的生物传感应用中展示了其能力。我们使用等温滴定量热法证明,当拆分成两条重叠的DNA链时,该适体仍具有功能。尺寸排阻色谱显示,与不存在配体时相比,结合奎宁的寡核苷酸形成了更大的适体单元组装体。最后,我们在奎宁的生物传感器应用中利用适体链寡核苷酸的寡聚物形成能力,使金纳米颗粒靠得更近,导致其等离子体共振向更长波长移动,并观察到颜色变化。我们提出,将适体拆分成在配体存在下形成寡聚物的重叠链,即适体链形成,通常适用于适体,并将在各种生物技术应用中证明是有用的。

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