A Systematic Assessment Of Current Genome-Scale Metabolic Reconstruction Tools

AbstractSeveral genome-scale metabolic reconstruction software platforms have been developed and are being continuously updated. These tools have been widely applied to reconstruct metabolic models for hundreds of microorganisms ranging from important human pathogens to species of industrial relevance. However, these platforms, as yet, have not been systematically evaluated with respect to software quality, best potential uses and intrinsic capacity to generate high-quality, genome-scale metabolic models. It is therefore unclear for potential users which tool best fits the purpose of their research. In this work, we performed a systematic assessment of the current genome-scale reconstruction software platforms. To meet our goal, we first defined a list of features for assessing software quality related to genome-scale reconstruction, which we expect to be useful for the potential users of these tools. Subsequently, we used the feature list to evaluate the performance of each tool. In order to assess the similarity of the draft reconstructions to high-quality models, we compared each tool’s output networks with that of the high-quality, manually curated, models of Lactobacillus plantarum and Bordetella pertussis, representatives of gram-positive and gram-negative bacteria, respectively. We showed that none of the tools outperforms the others in all the defined features and that model builders should carefully choose a tool (or combinations of tools) depending on the intended use of the metabolic model.Author SummaryMetabolic networks that comprise biochemical reactions at genome-scale have become very useful to study and predict the phenotype of important microorganisms. Several software platforms exist to build these metabolic networks. Based on different approaches and utilizing a variety of databases it is, unfortunately, unclear what are the best scenarios to use each of these tools. Hence, to understand the potential uses of these tools, we created a list of relevant features for metabolic reconstruction and we evaluated the tools in all these categories. Here, we show that none of the tools is better than the other in all the evaluated categories; instead, each tool is more suitable for particular purposes. Therefore, users should carefully select the tool(s) that best fit the purpose of their research. This is the first time these tools are systematically evaluated and this overview can be used as a guide for selecting the correct tool(s) for each case.

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Model-guided identification of novel gene amplification targets for improving succinate production in Escherichia coli NZN111

Integrative Biology ◽

10.1039/c7ib00077d ◽

2017 ◽

Vol 9 (10) ◽

pp. 830-835 ◽

Cited By ~ 2

Author(s):

Xingxing Jian ◽

Ningchuan Li ◽

Qian Chen ◽

Qiang Hua

Keyword(s):

Escherichia Coli ◽

Metabolic Engineering ◽

Gene Amplification ◽

Metabolic Networks ◽

Computational Analysis ◽

Succinate Production ◽

Novel Gene ◽

Metabolic Models ◽

Genome Scale

Reconstruction and application of genome-scale metabolic models (GEMs) have facilitated metabolic engineering by providing a platform on which systematic computational analysis of metabolic networks can be performed.

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Genome-scale reconstructions to assess metabolic phylogeny and organism clustering

PLoS ONE ◽

10.1371/journal.pone.0240953 ◽

2020 ◽

Vol 15 (12) ◽

pp. e0240953

Author(s):

Christian Schulz ◽

Eivind Almaas

Keyword(s):

Phylogenetic Trees ◽

Metabolic Networks ◽

Sulfur Metabolism ◽

Phylogenetic Analyses ◽

Tree Of Life ◽

Significant Heterogeneity ◽

Metabolic Reaction ◽

High Quality ◽

Conserved Genes ◽

Genome Scale

Approaches for systematizing information of relatedness between organisms is important in biology. Phylogenetic analyses based on sets of highly conserved genes are currently the basis for the Tree of Life. Genome-scale metabolic reconstructions contain high-quality information regarding the metabolic capability of an organism and are typically restricted to metabolically active enzyme-encoding genes. While there are many tools available to generate draft reconstructions, expert-level knowledge is still required to generate and manually curate high-quality genome-scale metabolic models and to fill gaps in their reaction networks. Here, we use the tool AutoKEGGRec to construct 975 genome-scale metabolic draft reconstructions encoded in the KEGG database without further curation. The organisms are selected across all three domains, and their metabolic networks serve as basis for generating phylogenetic trees. We find that using all reactions encoded, these metabolism-based comparisons give rise to a phylogenetic tree with close similarity to the Tree of Life. While this tree is quite robust to reasonable levels of noise in the metabolic reaction content of an organism, we find a significant heterogeneity in how much noise an organism may tolerate before it is incorrectly placed in the tree. Furthermore, by using the protein sequences for particular metabolic functions and pathway sets, such as central carbon-, nitrogen-, and sulfur-metabolism, as basis for the organism comparisons, we generate highly specific phylogenetic trees. We believe the generation of phylogenetic trees based on metabolic reaction content, in particular when focused on specific functions and pathways, could aid the identification of functionally important metabolic enzymes and be of value for genome-scale metabolic modellers and enzyme-engineers.

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A systematic assessment of current genome-scale metabolic reconstruction tools

Genome Biology ◽

10.1186/s13059-019-1769-1 ◽

2019 ◽

Vol 20 (1) ◽

Cited By ~ 28

Author(s):

Sebastián N. Mendoza ◽

Brett G. Olivier ◽

Douwe Molenaar ◽

Bas Teusink

Keyword(s):

Metabolic Reconstruction ◽

Systematic Assessment ◽

Genome Scale

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Genome Scale Constraint-Based Metabolic Reconstruction of Propionibacterium Freudenreichii DSM 20271

10.21203/rs.3.rs-847511/v1 ◽

2021 ◽

Author(s):

Mahsa Sadat Razavi Borghei ◽

Meysam Mobasheri ◽

Tabassom Sobati

Keyword(s):

Metabolic Networks ◽

Metabolic Model ◽

Physiological Data ◽

Metabolic Reconstruction ◽

Modeling And Analysis ◽

Microbial Cell Factories ◽

Culture Optimization ◽

Cell Factories ◽

Functional Features ◽

Genome Scale

Abstract Propionibacterium is an anaerobic bacterium with a history of use in the production of Swiss cheese and, more recently, several industrial bioproducts. While the use of this strain for the production of organic acids and secondary metabolites has gained growing interest, the industrial application of the strain requires further improvement in the yield and productivity of the target products. Systems modeling and analysis of metabolic networks are widely leveraged to gain holistic insights into the metabolic features of biotechnologically important strains and to devise metabolic engineering and culture optimization strategies for economically viable bioprocess development. In the present study, a high-quality genome-scale metabolic model of P. freudenreichii ssp. freudenreichii strain DSM 20271 was developed based on the strain’s genome annotation and biochemical and physiological data. The model covers the functions of 23% of the strain’s ORFs and accounts for 711 metabolic reactions and 647 unique metabolites. Literature-based reconstruction of the central metabolism and rigorous refinement of annotation data for establishing gene-protein-reaction associations renders the model a curated omic-scale knowledge base of the organism. Validation of the model against experimental data indicates that the reconstruction can capture the key structural and functional features of P. freudenreichii metabolism, including the growth rate, the pattern of flux distribution, the strain’s aerotolerance behavior, and the change in the mode of metabolic activity during the transition from an anaerobic to an aerobic growth regime. The model also includes an accurately curated pathway of cobalamin biosynthesis, which was used to examine the capacity of the strain to produce vitamin B12 precursors. Constraint-based reconstruction and analysis of the P. freudenreichii metabolic network also provided novel insights into the complexity and robustness of P. freudenreichii energy metabolism. The developed reconstruction, hence, may be used as a platform for the development of P. freudenreichii-based microbial cell factories and bioprocesses.

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Comparison of metabolic states using genome-scale metabolic models

PLoS Computational Biology ◽

10.1371/journal.pcbi.1009522 ◽

2021 ◽

Vol 17 (11) ◽

pp. e1009522

Author(s):

Chaitra Sarathy ◽

Marian Breuer ◽

Martina Kutmon ◽

Michiel E. Adriaens ◽

Chris T. Evelo ◽

...

Keyword(s):

Metabolic Networks ◽

Biological Significance ◽

Tca Cycle ◽

Cell Types ◽

Knowledge Bases ◽

Objective Functions ◽

Functional Differences ◽

Metabolic States ◽

Metabolic Models ◽

Genome Scale

Genome-scale metabolic models (GEMs) are comprehensive knowledge bases of cellular metabolism and serve as mathematical tools for studying biological phenotypes and metabolic states or conditions in various organisms and cell types. Given the sheer size and complexity of human metabolism, selecting parameters for existing analysis methods such as metabolic objective functions and model constraints is not straightforward in human GEMs. In particular, comparing several conditions in large GEMs to identify condition- or disease-specific metabolic features is challenging. In this study, we showcase a scalable, model-driven approach for an in-depth investigation and comparison of metabolic states in large GEMs which enables identifying the underlying functional differences. Using a combination of flux space sampling and network analysis, our approach enables extraction and visualisation of metabolically distinct network modules. Importantly, it does not rely on known or assumed objective functions. We apply this novel approach to extract the biochemical differences in adipocytes arising due to unlimited vs blocked uptake of branched-chain amino acids (BCAAs, considered as biomarkers in obesity) using a human adipocyte GEM (iAdipocytes1809). The biological significance of our approach is corroborated by literature reports confirming our identified metabolic processes (TCA cycle and Fatty acid metabolism) to be functionally related to BCAA metabolism. Additionally, our analysis predicts a specific altered uptake and secretion profile indicating a compensation for the unavailability of BCAAs. Taken together, our approach facilitates determining functional differences between any metabolic conditions of interest by offering a versatile platform for analysing and comparing flux spaces of large metabolic networks.

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Metabolic reconstruction, constraint-based analysis and game theory to probe genome-scale metabolic networks

Current Opinion in Biotechnology ◽

10.1016/j.copbio.2010.07.002 ◽

2010 ◽

Vol 21 (4) ◽

pp. 502-510 ◽

Cited By ~ 64

Author(s):

Eytan Ruppin ◽

Jason A Papin ◽

Luis F de Figueiredo ◽

Stefan Schuster

Keyword(s):

Game Theory ◽

Metabolic Networks ◽

Metabolic Reconstruction ◽

Genome Scale

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Software platforms to facilitate reconstructing genome-scale metabolic networks

Environmental Microbiology ◽

10.1111/1462-2920.12312 ◽

2013 ◽

Vol 16 (1) ◽

pp. 49-59 ◽

Cited By ~ 52

Author(s):

Joshua J. Hamilton ◽

Jennifer L. Reed

Keyword(s):

Metabolic Networks ◽

Software Platforms ◽

Genome Scale

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Modeling the Differences in Biochemical Capabilities ofPseudomonasSpecies by Flux Balance Analysis: How Good Are Genome-Scale Metabolic Networks at Predicting the Differences?

The Scientific World JOURNAL ◽

10.1155/2014/416289 ◽

2014 ◽

Vol 2014 ◽

pp. 1-11 ◽

Cited By ~ 6

Author(s):

Parizad Babaei ◽

Tahereh Ghasemi-Kahrizsangi ◽

Sayed-Amir Marashi

Keyword(s):

In Silico ◽

Metabolic Networks ◽

Closely Related Species ◽

Systematic Analysis ◽

Reconstruction Process ◽

Flux Balance ◽

Wide Range ◽

Balance Analysis ◽

Metabolic Models ◽

Genome Scale

To date, several genome-scale metabolic networks have been reconstructed. These models cover a wide range of organisms, from bacteria to human. Such models have provided us with a framework for systematic analysis of metabolism. However, little effort has been put towards comparing biochemical capabilities of closely related species using their metabolic models. The accuracy of a model is highly dependent on the reconstruction process, as some errors may be included in the model during reconstruction. In this study, we investigated the ability of threePseudomonasmetabolic models to predict the biochemical differences, namely, iMO1086, iJP962, and iSB1139, which are related toP. aeruginosaPAO1,P. putidaKT2440, andP. fluorescensSBW25, respectively. We did a comprehensive literature search for previous works containing biochemically distinguishable traits over these species. Amongst more than 1700 articles, we chose a subset of them which included experimental results suitable forin silicosimulation. By simulating the conditions provided in the actual biological experiment, we performed case-dependent tests to compare thein silicoresults to the biological ones. We found out that iMO1086 and iJP962 were able to predict the experimental data and were much more accurate than iSB1139.

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Genome-scale metabolic reconstruction of the stress-tolerant hybrid yeast Zygosaccharomyces parabailii

10.1101/373621 ◽

2018 ◽

Author(s):

Marzia Di Filippo ◽

Raúl A. Ortiz-Merino ◽

Chiara Damiani ◽

Gianni Frascotti ◽

Danilo Porro ◽

...

Keyword(s):

Laboratory Data ◽

Metabolic Model ◽

Cellular Systems ◽

Metabolic Reconstruction ◽

Genome Sequences ◽

Metabolic Potential ◽

Cell Factories ◽

Metabolic Models ◽

Constraint Based Modeling ◽

Genome Scale

Genome-scale metabolic models are powerful tools to understand and engineer cellular systems facilitating their use as cell factories. This is especially true for microorganisms with known genome sequences from which nearly complete sets of enzymes and metabolic pathways are determined, or can be inferred. Yeasts are highly diverse eukaryotes whose metabolic traits have long been exploited in industry, and although many of their genome sequences are available, few genome-scale metabolic models have so far been produced. For the first time, we reconstructed the genome-scale metabolic model of the hybrid yeast Zygosaccharomyces parabailii, which is a member of the Z. bailii sensu lato clade notorious for stress-tolerance and therefore relevant to industry. The model comprises 3096 reactions, 2091 metabolites, and 2413 genes. Our own laboratory data were then used to establish a biomass synthesis reaction, and constrain the extracellular environment. Through constraint-based modeling, our model reproduces the co-consumption and catabolism of acetate and glucose posing it as a promising platform for understanding and exploiting the metabolic potential of Z. parabailii.

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Suggestions for Standardized Identifiers for Fatty Acyl Compounds in Genome Scale Metabolic Models and Their Application to the WormJam Caenorhabditis elegans Model

Metabolites ◽

10.3390/metabo10040130 ◽

2020 ◽

Vol 10 (4) ◽

pp. 130

Author(s):

Michael Witting

Keyword(s):

Caenorhabditis Elegans ◽

Metabolic Networks ◽

Fatty Acid Biosynthesis ◽

Structural Information ◽

Current Knowledge ◽

Fatty Acyl ◽

Charge Balance ◽

Structural Annotation ◽

Metabolic Models ◽

Genome Scale

Genome scale metabolic models (GSMs) are a representation of the current knowledge on the metabolism of a given organism or superorganism. They group metabolites, genes, enzymes and reactions together to form a mathematical model and representation that can be used to analyze metabolic networks in silico or used for analysis of omics data. Beside correct mass and charge balance, correct structural annotation of metabolites represents an important factor for analysis of these metabolic networks. However, several metabolites in different GSMs have no or only partial structural information associated with them. Here, a new systematic nomenclature for acyl-based metabolites such as fatty acids, acyl-carnitines, acyl-coenzymes A or acyl-carrier proteins is presented. This nomenclature enables one to encode structural details in the metabolite identifiers and improves human readability of reactions. As proof of principle, it was applied to the fatty acid biosynthesis and degradation in the Caenorhabditis elegans consensus model WormJam.

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