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SEGMENTATION OF SES FOR PROTEIN STRUCTURE ANALYSIS

机译:蛋白质结构分析SES的分割

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The morphological complementarities of molecular surfaces provides insights for the identification and evaluation of binding sites. A quantitative characterization of these sites is an initial step towards protein based drug design. The final goal of the activity here presented is to provide a method that allows the identification of sites of possible protein-protein and protein-ligand interaction on the basis of the geometrical and topological structure of protein surfaces. The goal is to discover complementary regions (that is with concave and convex segments that match each others) among different molecules. In particular, we are considering the first step of this process: the segmentation of the protein surface in protuberances and cavities through an approach based on an analysis of the molecule Convex Hull and on the Distance Transform.
机译:分子表面的形态互补性为鉴定和评估结合位点提供了见解。这些位点的定量表征是朝向蛋白质的药物设计的初始步骤。这里呈现的活动的最终目标是提供一种方法,其允许基于蛋白质表面的几何和拓扑结构的基于几何和拓扑结构来鉴定可能的蛋白质和蛋白质 - 配体相互作用的方法。目标是在不同的分子中发现互补区域(与彼此相匹配的凹凸和凸片)。特别是,我们正在考虑该过程的第一步:通过基于分子凸壳和距离变换的分析,通过一种方法对突起和空腔进行蛋白质表面的分割。

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