The BioCyc database collection is an assortment of organism specific Pathway/Genome Databases (PGDBs) that provide reference to genome and metabolic pathway information for thousands of organisms.[1] As of July 2023, there were over 20,040 databases within BioCyc.[2] SRI International,[3] based in Menlo Park, California, maintains the BioCyc database family.
Content | |
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Description | Tools for navigating, visualizing, and analyzing the underlying databases, and for analyzing omics data |
Contact | |
Research center | SRI International |
Authors | Peter Karp et al |
Release date | 1997 |
Access | |
Website | biocyc |
Categories of Databases
editBased on the manual curation done, BioCyc database family is divided into 3 tiers:
Tier 1: Databases which have received at least one year of literature based manual curation. Currently there are seven databases in Tier 1. Out of the seven, MetaCyc is a major database that contains almost 2500 metabolic pathways from many organisms.[1][4] The other important Tier 1 database is HumanCyc which contains around 300 metabolic pathways found in humans.[5] The remaining five databases include, EcoCyc (E. coli),[6] AraCyc (Arabidopsis thaliana), YeastCyc (Saccharomyces cerevisiae), LeishCyc (Leishmania major Friedlin) and TrypanoCyc (Trypanosoma brucei).
Tier 2: Databases that were computationally predicted but have received moderate manual curation (most with 1–4 months curation). Tier 2 Databases are available for manual curation by scientists who are interested in any particular organism. Tier 2 databases currently contain 43 different organism databases.
Tier 3: Databases that were computationally predicted by PathoLogic and received no manual curation. As with Tier 2, Tier 3 databases are also available for curation for interested scientists.
Software tools
editThe BioCyc website contains a variety of software tools for searching, visualizing, comparing, and analyzing genome and pathway information. It includes a genome browser, and browsers for metabolic and regulatory networks. The website also includes tools for painting large-scale ("omics") datasets onto metabolic and regulatory networks, and onto the genome.
Use in Research
editSince BioCyc Database family comprises a long list of organism specific databases and also data at different systems level in a living system, the usage in research has been in a wide variety of context. Here, two studies are highlighted which show two different varieties of uses, one on a genome scale and other on identifying specific SNPs (Single Nucleotide Polymorphisms) within a genome.
AlgaGEM
AlgaGEM is a genome scale metabolic network model for a compartmentalized algae cell developed by Gomes de Oliveira Dal’Molin et al.[7] based on the Chlamydomonas reinhardtii genome. It has 866 unique ORFs, 1862 metabolites, 2499 gene-enzyme-reaction-association entries, and 1725 unique reactions. One of the Pathway databases used for reconstruction is MetaCyc.
SNPs
The study by Shimul Chowdhury et al.[8] showed association differed between maternal SNPs and metabolites involved in homocysteine, folate, and transsulfuration pathways in cases with Congenital Heart Defects (CHDs) as opposed to controls. The study used HumanCyc to select candidate genes and SNPs.
References
edit- ^ a b Caspi, R.; Altman, T.; Dreher, K.; Fulcher, C. A.; Subhraveti, P.; Keseler, I. M.; Kothari, A.; Krummenacker, M.; Latendresse, M.; Mueller, L. A.; Ong, Q.; Paley, S.; Pujar, A.; Shearer, A. G.; Travers, M.; Weerasinghe, D.; Zhang, P.; Karp, P. D. (2011). "The Meta Cyc database of metabolic pathways and enzymes and the Bio Cyc collection of pathway/genome databases". Nucleic Acids Research. 40 (Database issue): D742–53. doi:10.1093/nar/gkr1014. PMC 3245006. PMID 22102576.
- ^ "BioCyc Pathway/Genome Database Collection". biocyc.org. Retrieved 2023-07-31.
- ^ Home page of the SRI International
- ^ Karp, Peter D.; Caspi, Ron (2011). "A survey of metabolic databases emphasizing the Meta Cyc family". Archives of Toxicology. 85 (9): 1015–33. doi:10.1007/s00204-011-0705-2. PMC 3352032. PMID 21523460.
- ^ Romero, Pedro; Wagg, Jonathan; Green, Michelle L; Kaiser, Dale; Krummenacker, Markus; Karp, Peter D (2004). "Computational prediction of human metabolic pathways from the complete human genome". Genome Biology. 6 (1): R2. doi:10.1186/gb-2004-6-1-r2. PMC 549063. PMID 15642094.
- ^ Keseler, I. M.; Collado-Vides, J.; Santos-Zavaleta, A.; Peralta-Gil, M.; Gama-Castro, S.; Muniz-Rascado, L.; Bonavides-Martinez, C.; Paley, S.; Krummenacker, M.; Altman, T.; Kaipa, P.; Spaulding, A.; Pacheco, J.; Latendresse, M.; Fulcher, C.; Sarker, M.; Shearer, A. G.; MacKie, A.; Paulsen, I.; Gunsalus, R. P.; Karp, P. D. (2010). "Eco Cyc: A comprehensive database of Escherichia coli biology". Nucleic Acids Research. 39 (Database issue): D583–90. doi:10.1093/nar/gkq1143. PMC 3013716. PMID 21097882.
- ^ Dal'Molin, C. G.; Quek, L. E.; Palfreyman, R. W.; Nielsen, L. K. (2011). "AlgaGEM--a genome-scale metabolic reconstruction of algae based on the Chlamydomonas reinhardtii genome". BMC Genomics. 12 (Suppl 4): S5. doi:10.1186/1471-2164-12-S4-S5. PMC 3287588. PMID 22369158.
- ^ Chowdhury, S; Hobbs, C. A.; MacLeod, S. L.; Cleves, M. A.; Melnyk, S; James, S. J.; Hu, P; Erickson, S. W. (2012). "Associations between maternal genotypes and metabolites implicated in congenital heart defects". Molecular Genetics and Metabolism. 107 (3): 596–604. doi:10.1016/j.ymgme.2012.09.022. PMC 3523122. PMID 23059056.