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Reference: Karp PD, et al. (2013) Data mining in the MetaCyc family of pathway databases. Methods Mol Biol 939:183-200

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Abstract

Pathway databases collect the bioreactions and molecular interactions that define the processes of life. The MetaCyc family of pathway databases consists of thousands of databases that were derived through computational inference of metabolic pathways from the MetaCyc pathway/genome database (PGDB). In some cases, these DBs underwent subsequent manual curation. Curated pathway DBs are now available for most of the major model organisms. Databases in the MetaCyc family are managed using the Pathway Tools software. This chapter presents methods for performing data mining on the MetaCyc family of pathway DBs. We discuss the major data access mechanisms for the family, which include data files in multiple formats; application programming interfaces (APIs) for the Lisp, Java, and Perl languages; and web services. We present an overview of the Pathway Tools schema, an understanding of which is needed to query the DBs. The chapter also presents several interactive data mining tools within Pathway Tools for performing omics data analysis.

Reference Type
Journal Article | Research Support, N.I.H., Extramural
Authors
Karp PD, Paley S, Altman T
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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