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Global Alignment of Pairwise Protein Interaction Networks for Maximal Common Conserved Patterns

机译:成对蛋白质相互作用网络的最大共同保守模式的全局比对。

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摘要

A number of tools for the alignment of protein-protein interaction (PPI) networks have laid the foundation for PPI network analysis. Most of alignment tools focus on finding conserved interaction regions across the PPI networks through either local or global mapping of similar sequences. Researchers are still trying to improve the speed, scalability, and accuracy of network alignment. In view of this, we introduce a connected-components based fast algorithm, HopeMap, for network alignment. Observing that the size of true orthologs across species is small comparing to the total number of proteins in all species, we take a different approach based on a precompiled list of homologs identified by KO terms. Applying this approach to S. cerevisiae (yeast) and D. melanogaster (fly), E. coli K12 and S. typhimurium, E. coli K12 and C. crescenttus, we analyze all clusters identified in the alignment. The results are evaluated through up-to-date known gene annotations, gene ontology (GO), and KEGG ortholog groups (KO). Comparing to existing tools, our approach is fast with linear computational cost, highly accurate in terms of KO and GO terms specificity and sensitivity, and can be extended to multiple alignments easily.
机译:用于蛋白质-蛋白质相互作用(PPI)网络比对的许多工具为PPI网络分析奠定了基础。大多数比对工具都致力于通过相似序列的局部或全局映射,在整个PPI网络中寻找保守的相互作用区域。研究人员仍在尝试提高网络对齐的速度,可伸缩性和准确性。有鉴于此,我们介绍了一种基于连接组件的快速算法HopeMap,用于网络对齐。观察到跨物种的真实直向同源物的大小与所有物种中蛋白质的总数相比很小,我们基于通过KO术语鉴定的同源物的预编译列表,采用了不同的方法。将此方法应用于酿酒酵母(酵母)和黑腹果蝇(蝇),大肠杆菌K12和鼠伤寒沙门氏菌,大肠杆菌K12和新月形梭菌,我们分析了比对中发现的所有簇。通过最新的已知基因注释,基因本体论(GO)和KEGG直系同源基因组(KO)评估结果。与现有工具相比,我们的方法具有线性计算成本快,在KO和GO方面的特异性和灵敏度方面非常准确的特点,并且可以轻松扩展到多个比对。

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