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一个新型二硫键模式数据库及其在远缘同源物发现中的应用。

A novel database of disulfide patterns and its application to the discovery of distantly related homologs.

作者信息

van Vlijmen Herman W T, Gupta Abhas, Narasimhan Lakshmi S, Singh Juswinder

机构信息

Structural Informatics Group, Biogen Inc., 14 Cambridge Center, Cambridge, MA 02142, USA.

出版信息

J Mol Biol. 2004 Jan 23;335(4):1083-92. doi: 10.1016/j.jmb.2003.10.077.

Abstract

Disulfide bonds are conserved strongly among proteins of related structure and function. Despite the explosive growth of protein sequence databases and the vast numbers of sequence search tools, no tool exists to draw relations between the disulfide patterns of homologous proteins. We present a comprehensive database of disulfide bonding patterns and a search method to find proteins with similar disulfide patterns. The disulfide database was constructed using disulfide annotations extracted from SwissProt, and was expanded significantly from 16,736 to 94,499 disulfide-containing domains by an inference method that combines SwissProt annotations with Pfam multiple alignments. To search the database, we define a disulfide description, called the disulfide signature, which encodes both spacings between cysteine residues and cysteine connectivity. A web tool was developed that allows users to search for related disulfide patterns and for subpatterns resulting from the removal of one or more disulfides from the pattern. We explore the possibility of using disulfide pattern conservation to identify protein homologs that are undetectable by PSI-BLAST. Examples include the homology between a sea anemone antihypertensive/antiviral protein and a sea anemone neurotoxin, and the homology between tick anticoagulant peptide and bovine trypsin inhibitor. In both examples, there is a clear structural similarity and a functional relationship. We used the database to find structural homologs for the Cripto CFC domain. The identification of a von Willebrand Factor C (VWFC)-like domain agrees with its functional role and explains mutation data. We believe that the rapid increase in structure determinations arising from structural genomics efforts and advances in mass spectrometry techniques will greatly increase the number of disulfide annotations. This information will become a valuable resource for structural and functional annotations of proteins. The availability of a searchable disulfide pattern database will thus provide a powerful new addition to existing homolog discovery methods.

摘要

二硫键在具有相关结构和功能的蛋白质中高度保守。尽管蛋白质序列数据库呈爆炸式增长,且有大量的序列搜索工具,但尚无工具可用于描绘同源蛋白质二硫键模式之间的关系。我们提供了一个全面的二硫键连接模式数据库以及一种搜索方法,用于查找具有相似二硫键模式的蛋白质。该二硫键数据库是利用从SwissProt中提取的二硫键注释构建而成的,并通过一种将SwissProt注释与Pfam多重比对相结合的推理方法,从16736个含二硫键结构域大幅扩展至94499个。为了搜索该数据库,我们定义了一种二硫键描述,称为二硫键特征码,它对半胱氨酸残基之间的间距和半胱氨酸连接性进行编码。我们开发了一个网络工具,允许用户搜索相关的二硫键模式以及通过从模式中去除一个或多个二硫键而产生的子模式。我们探讨了利用二硫键模式保守性来识别PSI-BLAST无法检测到的蛋白质同源物的可能性。例如,海葵抗高血压/抗病毒蛋白与海葵神经毒素之间的同源性,以及蜱抗凝肽与牛胰蛋白酶抑制剂之间的同源性。在这两个例子中,都存在明显的结构相似性和功能关系。我们利用该数据库为Cripto CFC结构域寻找结构同源物。鉴定出的类血管性血友病因子C(VWFC)结构域与其功能作用相符,并解释了突变数据。我们相信,结构基因组学研究和质谱技术的进步所带来的结构测定的快速增加,将极大地增加二硫键注释的数量。这些信息将成为蛋白质结构和功能注释的宝贵资源。因此,一个可搜索的二硫键模式数据库的可用性将为现有的同源物发现方法提供一个强大的新补充。

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