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预制微凝胶-酶复合物的吸附作为构建基于微凝胶的酶生物传感器的新策略。

Adsorption of Preformed Microgel-Enzyme Complexes as a Novel Strategy toward Engineering Microgel-Based Enzymatic Biosensors.

作者信息

Sigolaeva Larisa V, Shalybkova Anna A, Sharifullin Timur Z, Pergushov Dmitry V

机构信息

Department of Chemistry, M.V. Lomonosov Moscow State University, Leninskie Gory 1/3, 119991 Moscow, Russia.

出版信息

Micromachines (Basel). 2023 Aug 18;14(8):1629. doi: 10.3390/mi14081629.

Abstract

A novel approach to surface modification, which consists of the adsorption of microgel-enzyme complexes preformed in solution, is highlighted. Accordingly, the microgel-enzyme complexes were formed due to the electrostatic interaction of the oppositely charged interacting components, that is, a cationic poly(-isopropylacrylamide)-based microgel and glucose oxidase taken as a model enzyme. The spontaneous adsorption of the prepared microgel-enzyme complexes, examined by means of quartz crystal microbalance with dissipation monitoring and atomic force microscopy, was observed, resulting in the formation of well-adhered microgel-enzyme coatings. Further, the preformed microgel-enzyme complexes were adsorbed onto the modified graphite-based screen-printed electrodes, and their enzymatic responses were determined by means of amperometry, demonstrating a remarkable analytical performance toward the quantification of β-D-glucose in terms of high sensitivity (0.0162 A × M × cm), a low limit of detection (1 μM), and an expanded linear range (1-2000 μM). The fabricated microgel-enzyme biosensor constructs were found to be very stable against manifold-repeated measurements. Finally, the pH- or salt-induced release of glucose oxidase from the adsorbed preformed microgel-enzyme complexes was demonstrated. The findings obtained for the microgel-enzyme coatings prepared via adsorption of the preformed microgel-enzyme complexes were compared to those found for the microgel-enzyme coatings fabricated via a previously exploited two-stage sequential adsorption, which includes the adsorption of the microgel first, followed by the electrostatic binding of glucose oxidase by the adsorbed microgel.

摘要

本文重点介绍了一种新型的表面改性方法,该方法包括吸附预先在溶液中形成的微凝胶 - 酶复合物。因此,微凝胶 - 酶复合物是由于带相反电荷的相互作用组分之间的静电相互作用而形成的,即基于阳离子聚( - 异丙基丙烯酰胺)的微凝胶和作为模型酶的葡萄糖氧化酶。通过具有耗散监测功能的石英晶体微天平以及原子力显微镜对制备的微凝胶 - 酶复合物的自发吸附进行了研究,观察到形成了附着力良好的微凝胶 - 酶涂层。此外,预先形成的微凝胶 - 酶复合物被吸附到改性石墨基丝网印刷电极上,并通过安培法测定其酶促响应,结果表明该复合物对β - D - 葡萄糖的定量分析具有显著性能,灵敏度高(0.0162 A × M × cm)、检测限低(1 μM)且线性范围宽(1 - 2000 μM)。所制备的微凝胶 - 酶生物传感器构建体在多次重复测量中表现出非常好的稳定性。最后,证明了pH或盐诱导吸附的预先形成的微凝胶 - 酶复合物释放葡萄糖氧化酶。将通过吸附预先形成的微凝胶 - 酶复合物制备的微凝胶 - 酶涂层的研究结果与通过先前采用的两阶段顺序吸附制备的微凝胶 - 酶涂层的研究结果进行了比较,后者包括首先吸附微凝胶,然后吸附的微凝胶通过静电结合葡萄糖氧化酶。

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