g2f as a Novel Tool to Find and Fill Gaps in Metabolic Networks

Authors

Daniel Osorio, Universidad Nacional de Colombia
Kelly Botero, Universidad Nacional de Colombia
Andrés Pinzón Velasco, Universidad Nacional de Colombia
Nicolás Mendoza-Mejía, Pontificia Universidad Javeriana
Felipe Rojas-Rodríguez, The Netherlands Cancer Institute - Antoni van Leeuwenhoek Hospital
George Barreto, University of Limerick
Janneth González, Pontificia Universidad Javeriana

Date of this Version

12-2021

Document Type

Article

Citation

The R Journal (December 2021) 13(2); Editor: Dianne Cook

Comments

Copyright 2021, The R Foundation. Open access material. License: CC BY 4.0 International

Abstract

During the building of a genome-scale metabolic model, there are several dead-end metabolites and substrates which cannot be imported, produced, nor used by any reaction incorporated in the network. The presence of these dead-end metabolites can block out the net flux of the objective function when it is evaluated through Flux Balance Analysis (FBA), and when it is not blocked, bias in the biological conclusions increase. In this aspect, the refinement to restore the connectivity of the network can be carried out manually or using computational algorithms. The g2f package was designed as a tool to find the gaps from dead-end metabolites and fill them from the stoichiometric reactions of a reference, filtering candidate reactions using a weighting function. Additionally, this algorithm allows downloading all the sets of gene-associated stoichiometric reactions for a specific organism from the KEGG database. Our package is compatible with both 4.0.0 and 3.6.0 R versions.