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蛋白质印迹凝胶的选择性及其与蛋白质性质的关系:计算机模拟研究。

The selectivity of protein-imprinted gels and its relation to protein properties: A computer simulation study.

作者信息

Yankelov Rami, Yungerman Irena, Srebnik Simcha

机构信息

Department of Chemical Engineering, Technion - Israel Institute of Technology, Haifa, Israel, 32000.

出版信息

J Mol Recognit. 2017 Jul;30(7). doi: 10.1002/jmr.2607. Epub 2017 Jan 23.

Abstract

Polymer-based protein recognition systems have enormous potential within clinical and diagnostic fields due to their reusability, biocompatibility, ease of manufacturing, and potential specificity. Imprinted polymer matrices have been extensively studied and applied as a simple technique for creating artificial polymer-based recognition gels for a target molecule. Although this technique has been proven effective when targeting small molecules (such as drugs), imprinting of proteins have so far resulted in materials with limited selectivity due to the large molecular size of the protein and aqueous environment. Using coarse-grained molecular simulation, we investigate the relation between protein makeup, polymer properties, and the selectivity of imprinted gels. Nonspecific binding that results in poor selectivity is shown to be strongly dependent on surface chemistry of the template and competitor proteins as well as on polymer chemistry. Residence time distributions of proteins diffusing within the gels provide a transparent picture of the relation between polymer constitution, protein properties, and the nonspecific interactions with the imprinted gel. The pronounced effect of protein surface chemistry on imprinted gel specificity is demonstrated.

摘要

基于聚合物的蛋白质识别系统因其可重复使用性、生物相容性、易于制造以及潜在的特异性,在临床和诊断领域具有巨大潜力。印迹聚合物基质已被广泛研究并用作一种创建针对目标分子的基于聚合物的人工识别凝胶的简单技术。尽管该技术在针对小分子(如药物)时已被证明有效,但由于蛋白质的大分子尺寸和水性环境,迄今为止蛋白质印迹产生的材料选择性有限。通过粗粒度分子模拟,我们研究了蛋白质组成、聚合物性质与印迹凝胶选择性之间的关系。导致选择性差的非特异性结合被证明强烈依赖于模板和竞争蛋白的表面化学以及聚合物化学。蛋白质在凝胶中扩散的停留时间分布提供了聚合物组成、蛋白质性质以及与印迹凝胶非特异性相互作用之间关系的清晰图景。蛋白质表面化学对印迹凝胶特异性的显著影响得到了证明。

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