k-OptForce: Integrating Kinetics with Flux Balance Analysis for Strain Design

Chowdhury, Anupam; Zomorrodi, Ali R.; Maranas, Costas D.

doi:10.1371/journal.pcbi.1003487

Cited by 123 publications

(99 citation statements)

References 109 publications

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“…The most recent effort in MIP-based CSOMs combines the kinetic descriptions of metabolic steps with traditional stoichiometric models to improve their predictive power and suggest more accurate designs (113). By bridging the gap between stoichiometric-and kinetic-based models (114), k-OptForce may represent a game changer and a new chassis for future CSOM development efforts.…”

Section: A Taxonomy For Computational Strain Optimization Methodsmentioning

confidence: 99%

In SilicoConstraint-Based Strain Optimization Methods: the Quest for Optimal Cell Factories

Maia

Rocha

2016

Microbiol Mol Biol Rev

116

107

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SUMMARYShifting from chemical to biotechnological processes is one of the cornerstones of 21st century industry. The production of a great range of chemicals via biotechnological means is a key challenge on the way toward a bio-based economy. However, this shift is occurring at a pace slower than initially expected. The development of efficient cell factories that allow for competitive production yields is of paramount importance for this leap to happen. Constraint-based models of metabolism, together within silicostrain design algorithms, promise to reveal insights into the best genetic design strategies, a step further toward achieving that goal. In this work, a thorough analysis of the mainin silicoconstraint-based strain design strategies and algorithms is presented, their application in real-world case studies is analyzed, and a path for the future is discussed.

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Section: A Taxonomy For Computational Strain Optimization Methodsmentioning

confidence: 99%

In SilicoConstraint-Based Strain Optimization Methods: the Quest for Optimal Cell Factories

Maia

Rocha

2016

Microbiol Mol Biol Rev

116

107

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“…OptStrain [67], OptReg [68], OptForce [72], k-OptForce [16], OptORF [44], CosMos [20] Omics data integration Transcriptome GIMME [5], iMAT [82], GIM 3 E [76], E-Flux [18], PROM [13], MADE [38], tFBA [90], RELATCH [45], TEAM [19], AdaM [89], GX-FBA [60], mCADRE [92], FCGs [43], EXAMO [75], TIGER [37] Proteome GIMMEp [6] Pathway prediction BNICE [29], Cho et al [14], RetroPath [11], PathPred [59], DESHARKY [74], BioPath [94], XTMS [12], GEM-Path [56] phenotype and gene essentiality [24]. Even further, taking advantage of a large set of genome sequences available for various E. coli strains, the GEMs for 55 E. coli strains were used to investigate the variations in gene, reaction and metabolite contents, and the capabilities to adapt to different nutritional environments among the strains [40].…”

Section: Genome-scale Metabolic Networkmentioning

confidence: 99%

“…When compared with OptForce for succinate production in E. coli, CosMos suggested new strategies which required fewer modifications and gave higher succinate yield. Recently, k-OptForce was developed by incorporating known kinetic information of metabolic reactions into the OptForce platform [16]. In a benchmark study on the overproduction of l-serine in E. coli, k-OptForce identified key regulatory bottlenecks that OptForce failed to predict and eliminated unnecessary genetic interventions predicted by OptForce [16].…”

Section: Prediction Of Target Genes To Be Up-or Down-regulatedmentioning

confidence: 99%

“…Recently, k-OptForce was developed by incorporating known kinetic information of metabolic reactions into the OptForce platform [16]. In a benchmark study on the overproduction of l-serine in E. coli, k-OptForce identified key regulatory bottlenecks that OptForce failed to predict and eliminated unnecessary genetic interventions predicted by OptForce [16]. k-OptForce also suggested genetic interventions leading to increased production of the target compound by alleviating the substratelevel inhibition of key enzymes, which was emphasized as an example demonstrating the benefit of integrating enzyme kinetic information into the stoichiometric model.…”

Section: Prediction Of Target Genes To Be Up-or Down-regulatedmentioning

confidence: 99%

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Applications of genome-scale metabolic network model in metabolic engineering

Kim

et al. 2015

Journal of Industrial Microbiology and Biotechnology

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Genome-scale metabolic network model (GEM) is a fundamental framework in systems metabolic engineering. GEM is built upon extensive experimental data and literature information on gene annotation and function, metabolites and enzymes so that it contains all known metabolic reactions within an organism. Constraint-based analysis of GEM enables the identification of phenotypic properties of an organism and hypothesis-driven engineering of cellular functions to achieve objectives. Along with the advances in omics, high-throughput technology and computational algorithms, the scope and applications of GEM have substantially expanded. In particular, various computational algorithms have been developed to predict beneficial gene deletion and amplification targets and used to guide the strain development process for the efficient production of industrially important chemicals. Furthermore, an Escherichia coli GEM was integrated with a pathway prediction algorithm and used to evaluate all possible routes for the production of a list of commodity chemicals in E. coli. Combined with the wealth of experimental data produced by high-throughput techniques, much effort has been exerted to add more biological contexts into GEM through the integration of omics data and regulatory network information for the mechanistic understanding and improved prediction capabilities. In this paper, we review the recent developments and applications of GEM focusing on the GEM-based computational algorithms available for microbial metabolic engineering.

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“…Couples production of the target product with growth Reduces the run time through successive linear programming BiMOMA [20] Identifies a set of KO strategies for overproduction of a target product Implements the homeostasis effect instead of optimal growth RobustKnock [79] Identifies a set of KO strategies for overproduction of a target product Couples production of the target product objective (i.e., bioengineering) with growth (i.e., biological) objective A three level optimization problem (max-min of target product production in outer problem and max of biomass production in the inner problem) k-OptForce [80] Integrates the available kinetic information Metabolite concentrations and enzyme abundance are constraints within the physiologically relevant ranges for reactions with available kinetic information Kamp and Klamt [81] Uses duality between elementary modes (EMs) and minimal cut sets (MCSs) This approach enumerates the smallest intervention strategies that ensure overproduction of a target product.…”

Section: Metabolic Tinker [9]mentioning

confidence: 99%

Advances in de novo strain design using integrated systems and synthetic biology tools

Khodayari

Chowdhury

et al. 2015

Current Opinion in Chemical Biology

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Recent efforts in expanding the range of biofuel and biorenewable molecules using microbial production hosts have focused on the introduction of non-native pathways in model organisms and the bio-prospecting of non-model organisms with desirable features. Current challenges lie in the assembly and coordinated expression of the (non-)native pathways and the elimination of competing pathways and undesirable regulation. Several systems and synthetic biology approaches providing contrasting top-down and bottom-up strategies, respectively, have been developed. In this review, we discuss recent advances in both in silico and experimental approaches for metabolic pathway design and engineering, with a critical assessment of their merits and remaining challenges.

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k-OptForce: Integrating Kinetics with Flux Balance Analysis for Strain Design

Cited by 123 publications

References 109 publications

In SilicoConstraint-Based Strain Optimization Methods: the Quest for Optimal Cell Factories

In SilicoConstraint-Based Strain Optimization Methods: the Quest for Optimal Cell Factories

Applications of genome-scale metabolic network model in metabolic engineering

Advances in de novo strain design using integrated systems and synthetic biology tools

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