IntelliGO: a new vector-based semantic similarity measure including annotation origin

被引:69
作者
Benabderrahmane, Sidahmed [1 ]
Smail-Tabbone, Malika [1 ]
Poch, Olivier [2 ]
Napoli, Amedeo [1 ]
Devignes, Marie-Dominique [1 ]
机构
[1] Nancy Univ, INRIA, CNRS, LORIA,Equipe Orpailleur, F-54506 Vandoeuvre Les Nancy, France
[2] IGBMC, CNRS UMR7104, LBGI, F-67404 Illkirch Graffenstaden, France
关键词
GENE-EXPRESSION DATA; ONTOLOGY TERMS; GO; DATABASE;
D O I
10.1186/1471-2105-11-588
中图分类号
Q5 [生物化学];
学科分类号
071010 ; 081704 ;
摘要
Background: The Gene Ontology (GO) is a well known controlled vocabulary describing the biological process, molecular function and cellular component aspects of gene annotation. It has become a widely used knowledge source in bioinformatics for annotating genes and measuring their semantic similarity. These measures generally involve the GO graph structure, the information content of GO aspects, or a combination of both. However, only a few of the semantic similarity measures described so far can handle GO annotations differently according to their origin (i.e. their evidence codes). Results: We present here a new semantic similarity measure called IntelliGO which integrates several complementary properties in a novel vector space model. The coefficients associated with each GO term that annotates a given gene or protein include its information content as well as a customized value for each type of GO evidence code. The generalized cosine similarity measure, used for calculating the dot product between two vectors, has been rigorously adapted to the context of the GO graph. The IntelliGO similarity measure is tested on two benchmark datasets consisting of KEGG pathways and Pfam domains grouped as clans, considering the GO biological process and molecular function terms, respectively, for a total of 683 yeast and human genes and involving more than 67,900 pair-wise comparisons. The ability of the IntelliGO similarity measure to express the biological cohesion of sets of genes compares favourably to four existing similarity measures. For inter-set comparison, it consistently discriminates between distinct sets of genes. Furthermore, the IntelliGO similarity measure allows the influence of weights assigned to evidence codes to be checked. Finally, the results obtained with a complementary reference technique give intermediate but correct correlation values with the sequence similarity, Pfam, and Enzyme classifications when compared to previously published measures. Conclusions: The IntelliGO similarity measure provides a customizable and comprehensive method for quantifying gene similarity based on GO annotations. It also displays a robust set-discriminating power which suggests it will be useful for functional clustering. Availability: An on-line version of the IntelliGO similarity measure is available at: http://bioinfo.loria.fr/Members/benabdsi/intelligo_project/
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页数:16
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