首页> 外文期刊>Journal of Molecular Biology >Automated structure-based prediction of functional sites in proteins: applications to assessing the validity of inheriting protein function from homology in genome annotation and to protein docking.
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Automated structure-based prediction of functional sites in proteins: applications to assessing the validity of inheriting protein function from homology in genome annotation and to protein docking.

机译:蛋白质功能位点的基于结构的自动化预测:用于评估从基因组注释中的同源性到蛋白质对接继承蛋白质功能的有效性的应用。

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摘要

A major problem in genome annotation is whether it is valid to transfer the function from a characterised protein to a homologue of unknown activity. Here, we show that one can employ a strategy that uses a structure-based prediction of protein functional sites to assess the reliability of functional inheritance. We have automated and benchmarked a method based on the evolutionary trace approach. Using a multiple sequence alignment, we identified invariant polar residues, which were then mapped onto the protein structure. Spatial clusters of these invariant residues formed the predicted functional site. For 68 of 86 proteins examined, the method yielded information about the observed functional site. This algorithm for functional site prediction was then used to assess the validity of transferring the function between homologues. This procedure was tested on 18 pairs of homologous proteins with unrelated function and 70 pairs of proteins with related function, and was shown to be 94 % accurate. This automated method could be linked to schemes for genome annotation. Finally, we examined the use of functional site prediction in protein-protein and protein-DNA docking. The use of predicted functional sites was shown to filter putative docked complexes with a discrimination similar to that obtained by manually including biological information about active sites or DNA-binding residues. Copyright 2001 Academic Press.
机译:基因组注释中的主要问题是将功能从已表征的蛋白质转移至未知活性的同系物是否有效。在这里,我们表明可以采用一种策略,该策略使用基于结构的蛋白质功能位点预测来评估功能继承的可靠性。我们已经基于进化跟踪方法对方法进行了自动化和基准测试。使用多序列比对,我们确定了不变的极性残基,然后将其定位到蛋白质结构上。这些不变残基的空间簇形成了预测的功能位点。对于检查的86种蛋白质中的68种,该方法产生了有关观察到的功能位点的信息。然后使用该用于功能位点预测的算法来评估在同源物之间转移功能的有效性。该方法在18对功能无关的同源蛋白和70对功能相关的蛋白上进行了测试,结果证明准确度为94%。该自动化方法可以链接到基因组注释方案。最后,我们检查了蛋白质-蛋白质和蛋白质-DNA对接中功能性位点预测的用途。结果表明,使用预测的功能位点可以过滤推定的对接复合物,其区别类似于通过人工添加有关活性位点或DNA结合残基的生物学信息而获得的区别。版权所有2001学术出版社。

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