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基于表位印迹的分子印迹聚合物:从分子相互作用到可利用的生物信息学资源,以寻找表位模板的探索之旅。

Molecularly imprinted polymers by epitope imprinting: a journey from molecular interactions to the available bioinformatics resources to scout for epitope templates.

机构信息

Indivenire Srl, via Alla Cascata 56/C, Povo, 38123, Trento, Italy.

Department of Biotechnology, University of Verona, Strada Le Grazie 15, 37134, Verona, Italy.

出版信息

Anal Bioanal Chem. 2021 Oct;413(24):6101-6115. doi: 10.1007/s00216-021-03409-1. Epub 2021 May 20.

Abstract

The molecular imprinting of proteins is the process of forming biomimetics with entailed protein-recognition by means of a template-assisted synthesis. Protein-imprinted polymers (pMIPs) have been successfully employed in separations, assays, sensors, and imaging. From a technical point of view, imprinting a protein is both costly, for protein expression and purification, and challenging, for the preservation of the protein's structural properties. In fact, the imprinting process needs to guarantee the preservation of the same protein three-dimensional conformation that later would be recognized. So far, the captivating idea to imprint just a portion of the protein, i.e., an epitope, instead of the whole, proved successful, offering reduced costs, compatibility with many synthetic conditions (solvents, pH, temperatures), and fine-tuning of the peptide sequence so to target specific physiological and functional conditions of the protein, such as post-translational modifications. Here, protein-protein interactions and the biochemical features of the epitopes are inspected, deriving lessons to prepare more effective pMIPs. Epitopes are categorized in linear or structured, immunogenic or not, located at the protein's surface or buried in its core and the imprinting strategies are discussed. Moreover, attention is given to freely available online bioinformatics resources that might offer key tools to gain further rationale amid the selection process of suitable epitopes templates.

摘要

蛋白质的分子印迹是一种通过模板辅助合成形成具有特定蛋白质识别能力的仿生材料的过程。蛋白质印迹聚合物(pMIP)已成功应用于分离、检测、传感器和成像。从技术角度来看,印迹蛋白质既昂贵(因为需要蛋白质表达和纯化),又具有挑战性(因为需要保持蛋白质的结构特性)。实际上,印迹过程需要保证随后被识别的相同蛋白质的三维构象得以保留。到目前为止,印迹蛋白质的一部分(即表位)而不是整个蛋白质的想法非常吸引人,因为它可以降低成本、与许多合成条件(溶剂、pH 值、温度)兼容,并对肽序列进行微调,以针对蛋白质的特定生理和功能条件,如翻译后修饰。在这里,检查了蛋白质-蛋白质相互作用和表位的生化特征,从中得出了制备更有效 pMIP 的经验教训。表位分为线性或结构、免疫原性或非免疫原性、位于蛋白质表面或埋藏在其核心中,讨论了印迹策略。此外,还关注了免费提供的在线生物信息学资源,这些资源可能为合适表位模板的选择过程提供关键工具,以获得更多的合理依据。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/45d7/8440283/3478bab2a81e/216_2021_3409_Fig1_HTML.jpg

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