scholarly journals Bridging the Gap between Fluxomics and Industrial Biotechnology

2010 ◽  
Vol 2010 ◽  
pp. 1-13 ◽  
Author(s):  
Xueyang Feng ◽  
Lawrence Page ◽  
Jacob Rubens ◽  
Lauren Chircus ◽  
Peter Colletti ◽  
...  
Keyword(s):  
Metabolic Flux Analysis ◽  
Metabolic Regulation ◽  
Metabolic Networks ◽  
Metabolic Flux ◽  
Enzymatic Reaction ◽  
Industrial Biotechnology ◽  
Flux Analysis ◽  
Potential Applications ◽  
Balance Analysis ◽  
Precise Prediction

Metabolic flux analysis is a vital tool used to determine the ultimate output of cellular metabolism and thus detect biotechnologically relevant bottlenecks in productivity.13C-based metabolic flux analysis (13C-MFA) and flux balance analysis (FBA) have many potential applications in biotechnology. However, noteworthy hurdles in fluxomics study are still present. First, several technical difficulties in both13C-MFA and FBA severely limit the scope of fluxomics findings and the applicability of obtained metabolic information. Second, the complexity of metabolic regulation poses a great challenge for precise prediction and analysis of metabolic networks, as there are gaps between fluxomics results and other omics studies. Third, despite identified metabolic bottlenecks or sources of host stress from product synthesis, it remains difficult to overcome inherent metabolic robustness or to efficiently import and express nonnative pathways. Fourth, product yields often decrease as the number of enzymatic steps increases. Such decrease in yield may not be caused by rate-limiting enzymes, but rather is accumulated through each enzymatic reaction. Fifth, a high-throughput fluxomics tool hasnot been developed for characterizing nonmodel microorganisms and maximizing their application in industrial biotechnology. Refining fluxomics tools and understanding these obstacles will improve our ability to engineer highlyefficient metabolic pathways in microbial hosts.

scholarly journals Physicochemical and metabolic constraints for thermodynamics-based stoichiometric modelling under mesophilic growth conditions

2020 ◽  
Author(s):  
Claudio Tomi-Andrino ◽  
Rupert Norman ◽  
Thomas Millat ◽  
Philippe Soucaille ◽  
Klaus Winzer ◽  
...  
Keyword(s):  
Experimental Data ◽  
Metabolic Flux Analysis ◽  
In Silico ◽  
Physicochemical Parameters ◽  
Metabolic Flux ◽  
Living Systems ◽  
Flux Analysis ◽  
Flux Balance ◽  
Metabolic Fluxes ◽  
Balance Analysis

AbstractMetabolic engineering in the post-genomic era is characterised by the development of new methods for metabolomics and fluxomics, supported by the integration of genetic engineering tools and mathematical modelling. Particularly, constraint-based stoichiometric models have been widely studied: (i) flux balance analysis (FBA) (in silico), and (ii) metabolic flux analysis (MFA) (in vivo). Recent studies have enabled the incorporation of thermodynamics and metabolomics data to improve the predictive capabilities of these approaches. However, an in-depth comparison and evaluation of these methods is lacking. This study presents a thorough analysis of two different in silico methods tested against experimental data (metabolomics and 13C-MFA) for the mesophile Escherichia coli. In particular, a modified version of the recently published matTFA toolbox was created, providing a broader range of physicochemical parameters. Validating against experimental data allowed the determination of the best physicochemical parameters to perform the TFA (Thermodynamics-based Flux Analysis). An analysis of flux pattern changes in the central carbon metabolism between 13C-MFA and TFA highlighted the limited capabilities of both approaches for elucidating the anaplerotic fluxes. In addition, a method based on centrality measures was suggested to identify important metabolites that (if quantified) would allow to further constrain the TFA. Finally, this study emphasised the need for standardisation in the fluxomics community: novel approaches are frequently released but a thorough comparison with currently accepted methods is not always performed.Author summaryBiotechnology has benefitted from the development of high throughput methods characterising living systems at different levels (e.g. concerning genes or proteins), allowing the industrial production of chemical commodities. Recently, focus has been placed on determining reaction rates (or metabolic fluxes) in the metabolic network of certain microorganisms, in order to identify bottlenecks hindering their exploitation. Two main approaches are commonly used, termed metabolic flux analysis (MFA) and flux balance analysis (FBA), based on measuring and estimating fluxes, respectively. While the influence of thermodynamics in living systems was accepted several decades ago, its application to study biochemical networks has only recently been enabled. In this sense, a multitude of different approaches constraining well-established modelling methods with thermodynamics has been suggested. However, physicochemical parameters are generally not properly adjusted to the experimental conditions, which might affect their predictive capabilities. In this study, we have explored the reliability of currently available tools by investigating the impact of varying said parameters in the simulation of metabolic fluxes and metabolite concentration values. Additionally, our in-depth analysis allowed us to highlight limitations and potential solutions that should be considered in future studies.

scholarly journals iMTBGO: An Algorithm for Integrating Metabolic Networks with Transcriptomes Based on Gene Ontology Analysis

2019 ◽  
Vol 20 (4) ◽  
pp. 252-259
Author(s):  
Zhitao Mao ◽  
Hongwu Ma
Keyword(s):  
Gene Expression ◽  
Metabolic Networks ◽  
Metabolic Flux ◽  
Network Models ◽  
Reaction Rates ◽  
Marker Genes ◽  
Published Data ◽  
Flux Analysis ◽  
Prediction Errors ◽  
Balance Analysis

Background:Constraint-based metabolic network models have been widely used in phenotypic prediction and metabolic engineering design. In recent years, researchers have attempted to improve prediction accuracy by integrating regulatory information and multiple types of “omics” data into this constraint-based model. The transcriptome is the most commonly used data type in integration, and a large number of FBA (flux balance analysis)-based integrated algorithms have been developed.Methods and Results:We mapped the Kcat values to the tree structure of GO terms and found that the Kcat values under the same GO term have a higher similarity. Based on this observation, we developed a new method, called iMTBGO, to predict metabolic flux distributions by constraining reaction boundaries based on gene expression ratios normalized by marker genes under the same GO term. We applied this method to previously published data and compared the prediction results with other metabolic flux analysis methods which also utilize gene expression data. The prediction errors of iMTBGO for both growth rates and fluxes in the central metabolic pathways were smaller than those of earlier published methods.Conclusion:Considering the fact that reaction rates are not only determined by genes/expression levels, but also by the specific activities of enzymes, the iMTBGO method allows us to make more precise predictions of metabolic fluxes by using expression values normalized based on GO.

scholarly journals Dynamic metabolic flux analysis of underdetermined and overdetermined metabolic networks

2016 ◽  
Vol 49 (26) ◽  
pp. 318-323
Author(s):  
Sofia Fernandes ◽  
Julien Robitaille ◽  
Georges Bastin ◽  
Mario Jolicoeur ◽  
Alain Vande Wouwer
Keyword(s):  
Metabolic Flux Analysis ◽  
Metabolic Networks ◽  
Metabolic Flux ◽  
Flux Analysis

scholarly journals Assessing and Resolving Model Misspecifications in Metabolic Flux Analysis

2017 ◽  
Author(s):  
Rudiyanto Gunawan ◽  
Sandro Hutter
Keyword(s):  
Metabolic Flux Analysis ◽  
Iterative Procedure ◽  
Metabolic Networks ◽  
Metabolic Flux ◽  
Statistical Tests ◽  
Chinese Hamster ◽  
Least Square ◽  
Flux Analysis ◽  
Stoichiometric Matrix ◽  
F Test

Background: Metabolic flux analysis (MFA) is an indispensable tool in metabolic engineering. The simplest variant of MFA relies on an overdetermined stoichiometric model of the cell’s metabolism under the pseudo-steady state assumption, to evaluate the intracellular flux distribution. Despite its long history, the issue of model error in the overdetermined MFA, particularly misspecifications of the stoichiometric matrix, has not received much attention. Method: We evaluated the performance of statistical tests from linear least square regressions, namely Ramsey RESET test, F-test and Lagrange multiplier test, in detecting model misspecifications in the overdetermined MFA, particularly missing reactions. We further proposed an iterative procedure using the F-test to correct such an issue. Result: Using Chinese hamster ovary and random metabolic networks, we demonstrated that: (1) a statistically significant regression does not guarantee high accuracy of the flux estimates, (2) the removal of a reaction with a low flux magnitude can cause disproportionately large biases in the flux estimates, (3) the F-test could efficiently detect missing reactions, and (4) the proposed iterative procedure could robustly resolve the omission of reactions. Conclusion: Our work demonstrated that statistical analysis and tests could be used to systematically assess, detect and resolve model misspecifications in the overdetermined MFA.

scholarly journals ReMatch: a web-based tool to construct, store and share stoichiometric metabolic models with carbon maps for metabolic flux analysis

2008 ◽  
Vol 5 (2) ◽  
Author(s):  
Esa Pitkänen ◽  
Arto Åkerlund ◽  
Ari Rantanen ◽  
Paula Jouhten ◽  
Esko Ukkonen
Keyword(s):  
Data Integration ◽  
Network Model ◽  
Metabolic Flux Analysis ◽  
Metabolic Networks ◽  
Metabolic Flux ◽  
Network Models ◽  
Flux Analysis ◽  
Stoichiometric Matrix ◽  
Web Based ◽  
Integration Problem

Summary ReMatch is a web-based, user-friendly tool that constructs stoichiometric network models for metabolic flux analysis, integrating user-developed models into a database collected from several comprehensive metabolic data resources, including KEGG, MetaCyc and CheBI. Particularly, ReMatch augments the metabolic reactions of the model with carbon mappings to facilitateThe construction of a network model consisting of biochemical reactions is the first step in most metabolic modelling tasks. This model construction can be a tedious task as the required information is usually scattered to many separate databases whose interoperability is suboptimal, due to the heterogeneous naming conventions of metabolites in different databases. Another, particularly severe data integration problem is faced inReMatch has been developed to solve the above data integration problems. First, ReMatch matches the imported user-developed model against the internal ReMatch database while considering a comprehensive metabolite name thesaurus. This, together with wild card support, allows the user to specify the model quickly without having to look the names up manually. Second, ReMatch is able to augment reactions of the model with carbon mappings, obtained either from the internal database or given by the user with an easy-touse tool.The constructed models can be exported into 13C-FLUX and SBML file formats. Further, a stoichiometric matrix and visualizations of the network model can be generated. The constructed models of metabolic networks can be optionally made available to the other users of ReMatch. Thus, ReMatch provides a common repository for metabolic network models with carbon mappings for the needs of metabolic flux analysis community. ReMatch is freely available for academic use at http://www.cs.helsinki.fi/group/sysfys/software/rematch/.

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