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首页> 外文期刊>Journal of Molecular Biology >Annotating nucleic Acid-binding function based on protein structure.
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Annotating nucleic Acid-binding function based on protein structure.

机译:基于蛋白质结构的核酸结合功能注释。

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摘要

Many of the targets of structural genomics will be proteins with little or no structural similarity to those currently in the database. Therefore, novel function prediction methods that do not rely on sequence or fold similarity to other known proteins are needed. We present an automated approach to predict nucleic-acid-binding (NA-binding) proteins, specifically DNA-binding proteins. The method is based on characterizing the structural and sequence properties of large, positively charged electrostatic patches on DNA-binding protein surfaces, which typically coincide with the DNA-binding-sites. Using an ensemble of features extracted from these electrostatic patches, we predict DNA-binding proteins with high accuracy. We show that our method does not rely on sequence or structure homology and is capable of predicting proteins of novel-binding motifs and protein structures solved in an unbound state. Our method can also distinguish NA-binding proteins from other proteins that have similar, large positive electrostatic patches on their surfaces, but that do not bind nucleic acids.
机译:结构基因组学的许多目标将是与数据库中的蛋白质几乎没有或没有结构相似性的蛋白质。因此,需要不依赖与其他已知蛋白质的序列或折叠相似性的新颖功能预测方法。我们提出了一种自动化的方法来预测核酸结合(NA结合)蛋白,特别是DNA结合蛋白。该方法基于表征DNA结合蛋白表面上通常带有DNA结合位点的大型带正电荷的静电贴片的结构和序列特性。使用从这些静电贴片中提取的特征集合,我们可以高精度预测DNA结合蛋白。我们表明,我们的方法不依赖于序列或结构的同源性,并且能够预测新型结合基序的蛋白质和以未结合状态解决的蛋白质结构。我们的方法还可以将NA结合蛋白与其他在表面具有相似的大正静电斑块但不结合核酸的蛋白区分开。

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