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用于筛选和鉴定与蛋白质受体结合的配体的核磁共振光谱技术。

NMR spectroscopy techniques for screening and identifying ligand binding to protein receptors.

作者信息

Meyer Bernd, Peters Thomas

机构信息

Institute for Organic Chemistry, University of Hamburg, Martin Luther King Platz 6, 20146 Hamburg, Germany.

出版信息

Angew Chem Int Ed Engl. 2003 Feb 24;42(8):864-90. doi: 10.1002/anie.200390233.

Abstract

Binding events of ligands to receptors are the key for an understanding of biological processes. Gaining insight into protein-protein and protein-ligand interactions in solution has recently become possible on an atomic level by new NMR spectroscopic techniques. These experiments identify binding events either by looking at the resonance signals of the ligand or the protein. Ideally, both techniques together deliver a complete picture of ligand binding to a receptor. The approaches discussed in this review allow screening of compound libraries as well as a detailed identification of the groups involved in the binding events. Also, characterization of the binding strength and kinetics is possible, competitive binding as well as allosteric effects can be identified, and it has even been possible to identify ligand binding to intact viruses and membrane-bound proteins.

摘要

配体与受体的结合事件是理解生物过程的关键。最近,通过新的核磁共振光谱技术,在原子水平上深入了解溶液中的蛋白质-蛋白质和蛋白质-配体相互作用已成为可能。这些实验通过观察配体或蛋白质的共振信号来识别结合事件。理想情况下,这两种技术结合起来可以提供配体与受体结合的完整图景。本综述中讨论的方法允许筛选化合物库,并详细识别参与结合事件的基团。此外,还可以表征结合强度和动力学,识别竞争性结合以及变构效应,甚至还可以识别配体与完整病毒和膜结合蛋白的结合。

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