重组抗体和MIP纳米颗粒对SARS-CoV-2刺突糖蛋白阻抗生物识别表面电行为的影响

Douglas Vieira Thomaz, Riccardo Goldoni, G. Tartaglia, C. Malitesta, E. Mazzotta
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引用次数: 4

摘要

电化学免疫传感器通常被描述为解决紧急流行病学需求的创新策略,例如检测SARS-CoV-2的主要生物标志物刺突糖蛋白。然而,有多种受体,尤其是重组抗体,可用于开发这些生物传感平台,很少有报道比较它们在分析设备设计和传感性能方面的适用性。因此,这篇简短的报告针对SARS-CoV-2的不同阻抗生物识别表面(BioS)的性能进行了简短而直接的研究,这些表面由三种常见的重组抗体和分子印迹聚合物(MIP)纳米颗粒(nanoMIP)制成。所选择的NanoMIP是由于它们对SARS-CoV-2刺突糖蛋白受体结合域(RBD)的选择性。结果表明,基于MUDA和EDC/NHS交联的表面修饰方案对每个被测受体的锚定都是成功的,每次修饰后EIS的Nyquist图的半圆直径增加,这表明Rct的增加是由于介电材料在导电表面的结合。此外,用于制作BioS和人工受体的单克隆抗体类型导致了非常不同的反应,其中RBD5305和基于nanomip的BioS在本文报道的条件下显示出最高的信号增量,这表明它们适合用于开发SARS-CoV-2刺突糖蛋白的阻抗性免疫传感器。
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Effect of Recombinant Antibodies and MIP Nanoparticles on the Electrical Behavior of Impedimetric Biorecognition Surfaces for SARS-CoV-2 Spike Glycoprotein: A Short Report
Electrochemical immunosensors are often described as innovative strategies to tackle urgent epidemiological needs, such as the detection of SARS-CoV-2 main biomarker, the spike glycoprotein. Nevertheless, there is a great variety of receptors, especially recombinant antibodies, that can be used to develop these biosensing platforms, and very few reports compare their suitability in analytical device design and their sensing performances. Therefore, this short report targeted a brief and straightforward investigation of the performance of different impedimetric biorecognition surfaces (BioS) for SARS-CoV-2, which were crafted from three commonly reported recombinant antibodies and molecularly-imprinted polymer (MIP) nanoparticles (nanoMIP). The selected NanoMIP were chosen due to their reported selectivity to the receptor binding domain (RBD) of SARS-CoV-2 spike glycoprotein. Results showed that the surface modification protocol based on MUDA and crosslinking with EDC/NHS was successful for the anchoring of each tested receptor, as the semicircle diameter of the Nyquist plots of EIS increased upon each modification, which suggests the increase of Rct due to the binding of dielectric materials on the conductive surface. Furthermore, the type of monoclonal antibody used to craft the BioS and the artificial receptors led to very distinct responses, being the RBD5305 and the NanoMIP-based BioS the ones that showcased the highest increment of signal in the conditions herein reported, which suggests their adequacy in the development of impedimetric immunosensors for SARS-CoV-2 spike glycoprotein.
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