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首页> 外文期刊>Journal of Medicinal Chemistry >Structural Artifacts in Protein-Ligand X-ray Structures: Implications for the Development of Docking Scoring Functions
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Structural Artifacts in Protein-Ligand X-ray Structures: Implications for the Development of Docking Scoring Functions

机译:蛋白质配体X射线结构中的结构伪像:对接计分功能发展的影响。

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The development of docking scoring functions requires high-resolution 3D structures of protein-ligand complexes for which the binding affinity of the ligand has been measured experimentally. Protein-ligand binding affinities are measured in solution experiments, and high resolution protein-ligand structures can be determined only by X-ray crystallography. Protein-ligand scoring functions must therefore reproduce solution binding energies using analyses of proteins in a crystal environment. We present an analysis of the prevalence of crystal-induced artifacts and water-mediated contacts in protein-ligand complexes and demonstrate the effect that these can have on the performance of protein-ligand scoring functions. We find 36% of ligands in the PDBBind 2007 refined data set to be influenced by crystal contacts and rind the performance of a scoring function to be affected by these. A Web server for detecting crystal contacts in protein-ligand complexes is available at http://enzyme.ucd.ie/LIGCRYST.
机译:对接评分功能的发展需要蛋白质-配体复合物的高分辨率3D结构,其配体的结合亲和力已通过实验测量。在溶液实验中测量蛋白质-配体结合亲和力,仅通过X射线晶体学即可确定高分辨率的蛋白质-配体结构。因此,蛋白质-配体评分功能必须使用晶体环境中的蛋白质分析来重现溶液结合能。我们目前对蛋白质-配体复合物中晶体诱导的假象和水介导的接触的普遍性进行分析,并证明它们可以对蛋白质-配体评分功能的性能产生影响。我们在PDBBind 2007精炼数据集中发现36%的配体受晶体接触的影响,而刻痕功能的性能受这些影响。可从http://enzyme.ucd.ie/LIGCRYST获得用于检测蛋白质-配体复合物中晶体接触的Web服务器。

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