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Finding of residues crucial for supersecondary structure formation

机译:寻找对超二级结构形成至关重要的残基

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This work evaluates the hypothesis that proteins with an identical supersecondary structure (SSS) share a unique set of residues-SSS-determining residues-even though they may belong to different protein families and have very low sequence similarities. This hypothesis was tested on two groups of sandwich-like proteins (SPs). Proteins in each group have an identical SSS, but their sequence similarity is below the "twilight zone." To find the SSS-determining residues specific to each group, a unique structure-based algorithm of multiple sequences alignment was developed. The units of alignment are individual strands and loops rather than whole sequences. The algorithm is based,on the alignment of residues that form hydrogen bonds between corresponding strands. Structure-based alignment revealed that 30-35% of the positions in the sequences in each group of proteins are "conserved positions" occupied either by hydrophobic-only or hydrophilic-only residues. Moreover, each group of SPs is characterized by a unique set of SSS-determining residues found at the conserved positions. The set of SSS-determining residues has very high sensitivity and specificity for identifying proteins with a corresponding SSS: It is an "amino acid tag" that brands a sequence as having a particular SSS. Thus, the sets of SSS-determining residues can be used to classify proteins and to predict the SSS of a query amino acid sequence.
机译:这项工作评估了一个假设,即具有相同超二级结构(SSS)的蛋白质共享一组独特的残基-确定SSS的残基-即使它们可能属于不同的蛋白质家族且序列相似性非常低。在两组三明治样蛋白(SPs)上测试了该假设。每组中的蛋白质具有相同的SSS,但它们的序列相似性低于“暮光区”。为了找到特定于每个组的SSS确定残基,开发了一种独特的基于结构的多序列比对算法。比对的单位是单独的链和环,而不是整个序列。该算法基于在相应链之间形成氢键的残基的比对。基于结构的比对显示,每组蛋白质中序列中30-35%的位置是“保守位置”,被仅疏水或仅亲水残基占据。而且,每组SP的特征在于在保守位置发现的一组独特的确定SSS的残基。确定SSS的残基集具有很高的灵敏度和特异性,可用于鉴定具有相应SSS的蛋白质:它是“氨基酸标签”,将序列标记为具有特定SSS。因此,确定SSS的残基组可用于分类蛋白质并预测查询氨基酸序列的SSS。

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