GPRuler: Metabolic gene-protein-reaction rules automatic reconstruction

Metabolic network models are increasingly being used in health care and industry. As a consequence, many tools have been released to automate their reconstruction process de novo. In order to enable gene deletion simulations and integration of gene expression data, these networks must include gene-p...

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Autores principales: Marzia Di Filippo, Chiara Damiani, Dario Pescini
Formato: article
Lenguaje:EN
Publicado: Public Library of Science (PLoS) 2021
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Acceso en línea:https://doaj.org/article/b4dee5e7cffb48888775f0d4e693746a
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Sumario:Metabolic network models are increasingly being used in health care and industry. As a consequence, many tools have been released to automate their reconstruction process de novo. In order to enable gene deletion simulations and integration of gene expression data, these networks must include gene-protein-reaction (GPR) rules, which describe with a Boolean logic relationships between the gene products (e.g., enzyme isoforms or subunits) associated with the catalysis of a given reaction. Nevertheless, the reconstruction of GPRs still remains a largely manual and time consuming process. Aiming at fully automating the reconstruction process of GPRs for any organism, we propose the open-source python-based framework GPRuler. By mining text and data from 9 different biological databases, GPRuler can reconstruct GPRs starting either from just the name of the target organism or from an existing metabolic model. The performance of the developed tool is evaluated at small-scale level for a manually curated metabolic model, and at genome-scale level for three metabolic models related to Homo sapiens and Saccharomyces cerevisiae organisms. By exploiting these models as benchmarks, the proposed tool shown its ability to reproduce the original GPR rules with a high level of accuracy. In all the tested scenarios, after a manual investigation of the mismatches between the rules proposed by GPRuler and the original ones, the proposed approach revealed to be in many cases more accurate than the original models. By complementing existing tools for metabolic network reconstruction with the possibility to reconstruct GPRs quickly and with a few resources, GPRuler paves the way to the study of context-specific metabolic networks, representing the active portion of the complete network in given conditions, for organisms of industrial or biomedical interest that have not been characterized metabolically yet. Author summary Over years, several methodologies have been proposed to integrate omics data into metabolic models in order to derive context-specific networks that represent the active portion of the network under specific conditions. In this way, biologically meaningful phenotypic predictions can be derived as a function of genes expression profiles encoding for subunits or isoforms of the involved enzymes. Regardless of the used approach to integrate omics data, the reliability of the formulated hypotheses strongly depends on the quality of gene-protein-reaction (GPR) rules included into the models, which describe how gene products concur to catalyze the associated reactions. To date, the reconstruction of GPR rules for their integration within metabolic networks still remains a largely manual and time consuming process. Therefore, we propose the open-source framework GPRuler to automate the reconstruction process of GPR rules for any living organism. Applying the developed tool to four case studies, we verified the ability of GPRuler to reproduce the original GPR rules with a very high level of accuracy. Moreover, in all the tested scenarios, the proposed approach revealed to be in many cases more accurate than the original models.