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SitCon: Binding Site Residue Conservation Visualization and Protein Sequence-to-Function Tool

机译:SitCon:结合位点残基保守性可视化和蛋白质序列转功能工具

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摘要

We introduce SitCon (SITe CONservation), a program designed to explore conservation of functionally important sites in a series of hypothetically homologous candidate protein structures, given amino acid sequence as an input. This can especially be useful when looking for an unknown function of a protein. SitCon exploits the fact that binding sites of proteins are preserved better than the overall residue sequence conservation. To test the capability of unknown function prediction, we randomly chose known function proteins from Caenorhabditis elegans genome. To imitate a behavior of an unknown function target, only the low homology proteins with 0.01 < E-score <= 100 were analyzed as templates. Out of 29 enzyme targets, SitCon was able to provide various hints about their function in at least 69% of the cases. For the eight nonenzyme targets, the predictions matched in only 25% of the cases. SitCon was also tested for a capability to predict presence or absence of metal-containing heterogroups in the target enzymes with -80% success rate. Because this algorithm is not based on specific protein signatures, it may allow detection of overlooked relationships between proteins. SitCon is also very effective as a tool allowing visual comparison of binding site residue conservation between the target and homologous templates side-by-side.
机译:我们引入SitCon(SITe保守性)程序,该程序旨在探索给定氨基酸序列作为输入的一系列假设同源候选蛋白质结构中功能重要位点的保守性。当寻找蛋白质的未知功能时,这尤其有用。 SitCon利用了这样一个事实,即蛋白质的结合位点比整体残基序列的保守性更好。为了测试未知功能预测的能力,我们从秀丽隐杆线虫基因组中随机选择了已知功能蛋白。为了模仿未知功能目标的行为,仅将0.01

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