The effects of model complexity and size on metabolic flux distribution and control: case study in Escherichia coli

, ,
BMC, 2021
Article

Résumé

Background Significant efforts have been made in building large-scale kinetic models of cellular metabolism in the past two decades. However, most kinetic models published to date, remain focused around central carbon pathways or are built around ad hoc reduced models without clear justification on their derivation and usage. Systematic algorithms exist for reducing genome-scale metabolic reconstructions to build thermodynamically feasible and consistently reduced stoichiometric models. However, it is important to study how network complexity affects conclusions derived from large-scale kinetic models built around consistently reduced models before we can apply them to study biological systems. Results We reduced the iJO1366 Escherichia Coli genome-scale metabolic reconstruction systematically to build three stoichiometric models of different size. Since the reduced models are expansions around the core subsystems for which the reduction was performed, the models are nested. We present a method for scaling up the flux profile and the concentration vector reference steady-states from the smallest model to the larger ones, whilst preserving maximum equivalency. Populations of kinetic models, preserving similarity in kinetic parameters, were built around the reference steady-states and their metabolic sensitivity coefficients (MSCs) were computed. The MSCs were sensitive to the model complexity. We proposed a metric for measuring the sensitivity of MSCs to these structural changes. Conclusions We proposed for the first time a workflow for scaling up the size of kinetic models while preserving equivalency between the kinetic models. Using this workflow, we demonstrate that model complexity in terms of networks size has significant impact on sensitivity characteristics of kinetic models. Therefore, it is essential to account for the effects of network complexity when constructing kinetic models. The presented metric for measuring MSC sensitivity to structural changes can guide modelers and experimentalists in improving model quality and guide synthetic biology and metabolic engineering. Our proposed workflow enables the testing of the suitability of a kinetic model for answering certain study-specific questions. We argue that the model-based metabolic design targets that are common across models of different size are of higher confidence, while those that are different could be the objective of investigations for model improvement.

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, ,
BMC, 2021
Article

Résumé

Official source

À propos de ce résultat

Concepts associés (13)

Concepts associés

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Publications associées (32)

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Exploring enhancement of 1,4-butanediol production in recombinant E. coli using large-scale kinetic models

Stefano Andreozzi, Anirikh Chakrabarti, Vassily Hatzimanikatis, Ljubisa Miskovic, Keng Cher Soh

Engineering of microbial cell factories requires a simultaneous optimization of several criteria such as productivity, yield, titer, stress tolerance, all the while retaining the efficient, cost-effective and robust process. One of the most prominent examples where a rational metabolic engineering strategy played a key role is in the production of 1,4-butanediol (BDO) in E. coli. In this study, we used the ORACLE (Optimization and Risk Analysis of Complex Living Entities) framework to analyze the physiology of metabolically engineered E. coli producing 1,4-butanediol (BDO) and to identify potential strategies for improved production of BDO. The framework allowed us to integrate data across multiple levels and to construct a population of large-scale kinetic models despite the lack of available information about kinetic properties of every enzyme in the metabolic pathways. We analyzed the population of these models and we found that the enzymes that primarily control the fluxes leading to BDO production are part of central glycolysis, the lower branch of tricarboxylic acid cycle and the novel BDO production route. We also identified targets for metabolic engineering for improved BDO production and yield, while constraining other intracellular states within desired bounds. We further analyzed these models to predict the effects of changes of the target enzymes on other intracellular states like energy charge, cofactor levels, redox state, cellular growth and byproduct formation. The conclusions of the performed analysis are consistent with the experimentally tested designs, and these results demonstrate the potential and effectiveness of ORACLE for the design of microbial cell factories.

2015

Chargement

Metabolic control analysis of the central carbon pathway in optimally grown E. coli

Stefano Andreozzi, Vassily Hatzimanikatis, Ljubisa Miskovic, Keng Cher Soh

The engineering of the metabolism requires the building of reliable kinetic models of the metabolic pathways through the integration of the information from heterogeneous data sources. Unfortunately, the quantitative knowledge about fluxes, mechanisms or kinetic parameters of the constituent reactions of the metabolic network is most of the times uncertain or missing, due to limitations in the measurement techniques of the relevant biological properties of the cell and variability in experimental conditions. In this contribution, we employ ORACLE (Optimization and Risk Analysis of Complex Living Entities), the computational framework for the analysis and optimization of metabolic networks that addresses these issues. ORACLE allows us to generate populations of kinetic models that account explicitly for the physico-chemical and thermodynamic features and constraints of metabolic networks. We show how ORACLE incorporates fluxomics and metabolomics data and constraints into the central carbon core model of E. coli to uncover its possible steady state behaviors, when the cells are cultivated under the physiological condition of optimal growth on different carbon sources, both anaerobically and aerobically. Alternative cases of possible intracellular flux and thermodynamic states, corresponding to the given experimental data, are identified and subsequently the kinetic analysis is performed to evaluate how the control over fluxes and concentrations is distributed over the metabolic network. We demonstrate that ORACLE methodology provides guidance for metabolic engineering in spite of uncertain/missing information in the local/global properties of the metabolic network, integrating a statistical account on the semi-quantitative available data with consistent thermodynamic information and plausible hypotheses.

2012

Chargement

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Kinetic models of metabolism can be constructed to predict cellular regulation and devise metabolic engineering strategies, and various promising computational workflows have been developed in recent years for this. Due to the uncertainty in the kinetic parameter values required to build kinetic models, these workflows rely on ensemble modeling (EM) principles for sampling and building populations of models describing observed physiologies. Sensitivity coefficients from metabolic control analysis (MCA) of kinetic models can provide important insight about cellular control around a given physiological steady state. However, despite considering populations of kinetic models and their model outputs, current approaches do not provide adequate tools for statistical inference. To derive conclusions from model outputs, such as MCA sensitivity coefficients, it is necessary to rank/compare populations of variables with each other. Currently existing workflows consider confidence intervals (CIs) that are derived independently for each comparable variable. Hence, it is important to derive simultaneous CIs for the variables that we wish to rank/compare. Herein, we used an existing large-scale kinetic model of Escherichia Coli metabolism to present how univariate CIs can lead to incorrect conclusions, and we present a new workflow that applies three different multivariate statistical approaches. We use the Bonferroni and the exact normal methods to build symmetric CIs using the normality assumptions. We then suggest how bootstrapping can compute asymmetric CIs whilst relaxing this normality assumption. We conclude that the Bonferroni and the exact normal methods can provide simple and efficient ways for constructing reliable CIs, with the exact normal method favored over the Bonferroni when the compared variables present dependencies. Bootstrapping, despite its significantly higher computational cost, is recommended when comparing non-normal distributions of variables. Additionally, we show how the Bonferroni method can readily be used to estimate required sample numbers to attain a certain CI size.

2019

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2019