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Reference: Misra S and Ray SS (2017) Finding optimum width of discretization for gene expressions using functional annotations. Comput Biol Med 90:59-67

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Abstract

Discretizing gene expression values is an important step in data preprocessing as it helps in reducing noise and experimental errors. This in turn provides better results in various tasks such as gene regulatory network analysis and disease prediction. A supervised discretization method for gene expressions using gene annotation is developed. The method is called "Gene Annotation Based Discretization" (GABD) where the discretization width is determined by maximizing the positive predictive value (PPV), computed using gene annotations, for top 20,000 gene pairs. The method can capture the gene similarity better than those obtained using original expressions. The performance of GABD is compared with some existing discretization methods like equal width discretization, equal frequency discretization and k-means discretization in terms of positive predictive value (PPV). The utility of GABD is also shown by clustering genes using k-medoid algorithm and thereby predicting the function of 23 unclassified Saccharomyces cerevisiae genes using p-value cut off 10-10. The source code for GABD is available at http://www.sampa.droppages.com/GABD.html.

Reference Type
Journal Article
Authors
Misra S, Ray SS
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Gene Ontology Annotations

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Gene/Complex Qualifier Gene Ontology Term Aspect Annotation Extension Evidence Method Source Assigned On Reference

Phenotype Annotations

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Gene Phenotype Experiment Type Mutant Information Strain Background Chemical Details Reference

Disease Annotations

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Gene Disease Ontology Term Qualifier Evidence Method Source Assigned On Reference

Regulation Annotations

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Regulator Target Direction Regulation Of Happens During Method Evidence

Post-translational Modifications

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Site Modification Modifier Reference

Interaction Annotations

Genetic Interactions

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Interactor Interactor Allele Assay Annotation Action Phenotype SGA score P-value Source Reference

Physical Interactions

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Interactor Interactor Assay Annotation Action Modification Source Reference

Functional Complementation Annotations

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Gene Species Gene ID Strain background Direction Details Source Reference

Published Datasets

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Dataset Description Keywords Number of Conditions Reference