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首页> 外文期刊>Proteins: Structure, Function, and Genetics >Assigning new GO annotations to protein data bank sequences by combining structure and sequence homology.
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Assigning new GO annotations to protein data bank sequences by combining structure and sequence homology.

机译:通过结合结构和序列同源性为蛋白质数据库序列分配新的GO注释。

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摘要

Accompanying the discovery of an increasing number of proteins, there is the need to provide functional annotation that is both highly accurate and consistent. The Gene Ontology (GO) provides consistent annotation in a computer readable and usable form; hence, GO annotation (GOA) has been assigned to a large number of protein sequences based on direct experimental evidence and through inference determined by sequence homology. Here we show that this annotation can be extended and corrected for cases where protein structures are available. Specifically, using the Combinatorial Extension (CE) algorithm for structure comparison, we extend the protein annotation currently provided by GOA at the European Bioinformatics Institute (EBI) to further describe the contents of the Protein Data Bank (PDB). Specific cases of biologically interesting annotations derived by this method are given. Given that the relationship between sequence, structure, and function is complicated, we explore the impact of this relationship on assigning GOA. The effect of superfolds (folds with many functions) is considered and, by comparison to the Structural Classification of Proteins (SCOP), the individual effects of family, superfamily, and fold.
机译:伴随发现越来越多的蛋白质,需要提供高度准确和一致的功能注释。基因本体(GO)以计算机可读和可用的形式提供一致的注释;因此,基于直接的实验证据并通过序列同源性确定的推论,GO注释(GOA)已分配给大量蛋白质序列。在这里,我们显示可以对蛋白质结构可用的情况进行扩展和纠正。具体来说,使用组合扩展(CE)算法进行结构比较,我们扩展了欧洲生物信息学研究所(EBI)GOA当前提供的蛋白质注释,以进一步描述蛋白质数据库(PDB)的内容。给出了通过这种方法获得的具有生物学意义的注释的具体案例。鉴于序列,结构和功能之间的关系很复杂,我们探讨了这种关系对分配GOA的影响。考虑了超折叠(具有许多功能的折叠)的作用,并且与蛋白质的结构分类(SCOP)相比,还考虑了家族,超家族和折叠的个体作用。

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