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首页> 外文期刊>BioMed research international >Predicting Flavin and Nicotinamide Adenine Dinucleotide-Binding Sites in Proteins Using the Fragment Transformation Method
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Predicting Flavin and Nicotinamide Adenine Dinucleotide-Binding Sites in Proteins Using the Fragment Transformation Method

机译:使用碎片转化方法预测蛋白质中的黄素和烟碱腺嘌呤二核苷酸结合位点

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摘要

We developed a computational method to identify NAD- and FAD-binding sites in proteins. First, we extracted from the Protein Data Bank structures of proteins that bind to at least one of these ligands. NAD-/FAD-binding residue templates were then constructed by identifying binding residues through the ligand-binding database BioLiP. The fragment transformation method was used to identify structures within query proteins that resembled the ligand-binding templates. By comparing residue types and their relative spatial positions, potential binding sites were identified and a ligand-binding potential for each residue was calculated. Setting the false positive rate at 5%, our method predicted NAD- and FAD-binding sites at true positive rates of 67.1% and 68.4%, respectively. Our method provides excellent results for identifying FAD- and NAD-binding sites in proteins, and the most important is that the requirement of conservation of residue types and local structures in the FAD- and NAD-binding sites can be verified.
机译:我们开发了一种计算方法,用于鉴定蛋白质中的NAD和FAD结合位点。首先,我们从与这些配体中的至少一种结合的蛋白质数据库结构中提取。然后通过鉴定通过配体结合数据库Biolip的结合残基来构建NAD- / FAD结合残留物模板。片段转化方法用于鉴定类似于配体结合模板的查询蛋白内的结构。通过比较残留物类型及其相对空间位置,鉴定潜在的结合位点,并计算每个残基的配体结合电位。将假阳性率为5%,我们的方法以真正的阳性率预测NAD-和FAD结合位点,分别为67.1%和68.4%。我们的方法提供了蛋白质中鉴定Fad-和NAD结合位点的优异结果,最重要的是可以验证残留物类型和局部结构的保存要求。

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