The FTMap family of web servers for determining and characterizing ligand-binding hot spots of proteins

可药性 配体(生物化学) 计算生物学 Web服务器 灵活性(工程) 小分子 蛋白质数据库 服务器 蛋白质配体 化学 计算机科学 蛋白质结构 生物 生物化学 基因 统计 互联网 万维网 受体 数学
作者
Dima Kozakov,Laurie E. Grove,David R. Hall,Tanggis Bohnuud,Scott E. Mottarella,Lingqi Luo,Bing Xia,Dmitri Beglov,Sándor Vajda
出处
期刊:Nature Protocols [Springer Nature]
卷期号:10 (5): 733-755 被引量:554
标识
DOI:10.1038/nprot.2015.043
摘要

This protocol describes the FTMap family of web servers for determining and characterizing ligand-binding hot spots of macromolecules, including FTSite for predicting ligand-binding sites, FTFlex for accounting for side chain flexibility, FTMap/param for parameterizing additional probes, and FTDyn for mapping ensembles of protein structures. FTMap is a computational mapping server that identifies binding hot spots of macromolecules—i.e., regions of the surface with major contributions to the ligand-binding free energy. To use FTMap, users submit a protein, DNA or RNA structure in PDB (Protein Data Bank) format. FTMap samples billions of positions of small organic molecules used as probes, and it scores the probe poses using a detailed energy expression. Regions that bind clusters of multiple probe types identify the binding hot spots in good agreement with experimental data. FTMap serves as the basis for other servers, namely FTSite, which is used to predict ligand-binding sites, FTFlex, which is used to account for side chain flexibility, FTMap/param, used to parameterize additional probes and FTDyn, for mapping ensembles of protein structures. Applications include determining the druggability of proteins, identifying ligand moieties that are most important for binding, finding the most bound-like conformation in ensembles of unliganded protein structures and providing input for fragment-based drug design. FTMap is more accurate than classical mapping methods such as GRID and MCSS, and it is much faster than the more-recent approaches to protein mapping based on mixed molecular dynamics. By using 16 probe molecules, the FTMap server finds the hot spots of an average-size protein in <1 h. As FTFlex performs mapping for all low-energy conformers of side chains in the binding site, its completion time is proportionately longer.
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