Three‐level hybrid modeling for systematic optimization of biocatalytic synthesis: α‐glucosyl glycerol production by enzymatic trans‐glycosylation from sucrose

Sigg, Alexander; Klimacek, Mario; Nidetzky, Bernd

doi:10.1002/bit.27878

Cited by 6 publications

(11 citation statements)

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“…The apparent violation of mass balance is explainable by enzymatic hydrolysis of Suc, G1P or both happening in small degree. ScP is known to possess low hydrolase activity towards Suc conditions in which the [Pi] is strongly limiting in the reaction (Klimacek et al, 2020; Sigg et al, 2021). However, as it did not affect the Cb formation, the side reaction leading to excess Glc in the process was not further investigated here.…”

Section: Resultsmentioning

confidence: 99%

“…A more robust approach uses design of experiments which can be performed in a purely data-driven fashion based on statistical models or under support from kinetic models of the synthetic reactions (Siedentop et al, 2021;Taylor, Pomberger, et al, 2023). Mechanism-based kinetic models achieve the most comprehensive and in-depth description of the reactions analyzed (Almquist et al, 2014;Gernaey et al, 2010;Harris et al, 2022;Sigg et al, 2021Sigg et al, , 2023. These models are powerful engineering tools of optimization in their own right.…”

Section: Introductionmentioning

confidence: 99%

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Pushing the boundaries of phosphorylase cascade reaction for cellobiose production II: Model‐based multiobjective optimization

Sigg,

Klimacek,

Nidetzky

2023

Biotech & Bioengineering

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The inherent complexity of coupled biocatalytic reactions presents a major challenge for process development with one‐pot multienzyme cascade transformations. Kinetic models are powerful engineering tools to guide the optimization of cascade reactions towards a performance suitable for scale up to an actual production. Here, we report kinetic model‐based window of operation analysis for cellobiose production (≥100 g/L) from sucrose and glucose by indirect transglycosylation via glucose 1‐phosphate as intermediate. The two‐step cascade transformation is catalyzed by sucrose and cellobiose phosphorylase in the presence of substoichiometric amounts of phosphate (≤27 mol% of substrate). Kinetic modeling was instrumental to uncover the hidden effect of bulk microviscosity due to high sugar concentrations on decreasing the rate of cellobiose phosphorylase specifically. The mechanistic‐empirical hybrid model thus developed gives a comprehensive description of the cascade reaction at industrially relevant substrate conditions. Model simulations serve to unravel opposed relationships between efficient utilization of the enzymes and maximized concentration (or yield) of the product within a given process time, in dependence of the initial concentrations of substrate and phosphate used. Optimum balance of these competing key metrics of process performance is suggested from the model‐calculated window of operation and is verified experimentally. The evidence shown highlights the important use of kinetic modeling for the characterization and optimization of cascade reactions in ways that appear to be inaccessible to purely data‐driven approaches.

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Section: Resultsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Pushing the boundaries of phosphorylase cascade reaction for cellobiose production II: Model‐based multiobjective optimization

Sigg,

Klimacek,

Nidetzky

2023

Biotech & Bioengineering

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“…Given this fundamental relevance of modeling, surprisingly, there seems to be a certain vagueness on its systematic use for practical effect in reaction development and optimization (for reviews, see Kara & Rudroff 2021; Siedentop et al, 2021). Analogous to experiment, kinetic models differ widely in the degree and detail of system description reached (Berendsen et al, 2006; Klimacek et al, 2020; Sigg et al, 2021; Sun et al, 2021). Central questions, like that of minimum model requirements for reliable application in cascade optimization, appear to lack authoritative answers.…”

Section: Introductionmentioning

confidence: 99%

Pushing the boundaries of phosphorylase cascade reaction for cellobiose production I: Kinetic model development

Sigg,

Klimacek,

Nidetzky

2023

Biotech & Bioengineering

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One‐pot cascade reactions of coupled disaccharide phosphorylases enable an efficient transglycosylation via intermediary α‐d‐glucose 1‐phosphate (G1P). Such transformations have promising applications in the production of carbohydrate commodities, including the disaccharide cellobiose for food and feed use. Several studies have shown sucrose and cellobiose phosphorylase for cellobiose synthesis from sucrose, but the boundaries on transformation efficiency that result from kinetic and thermodynamic characteristics of the individual enzyme reactions are not known. Here, we assessed in a step‐by‐step systematic fashion the practical requirements of a kinetic model to describe cellobiose production at industrially relevant substrate concentrations of up to 600 mM sucrose and glucose each. Mechanistic initial‐rate models of the two‐substrate reactions of sucrose phosphorylase (sucrose + phosphate → G1P + fructose) and cellobiose phosphorylase (G1P + glucose → cellobiose + phosphate) were needed and additionally required expansion by terms of glucose inhibition, in particular a distinctive two‐site glucose substrate inhibition of the cellobiose phosphorylase (fromCellulumonas uda). Combined with mass action terms accounting for the approach to equilibrium, the kinetic model gave an excellent fit and a robust prediction of the full reaction time courses for a wide range of enzyme activities as well as substrate concentrations, including the variable substoichiometric concentration of phosphate. The model thus provides the essential engineering tool to disentangle the highly interrelated factors of conversion efficiency in the coupled enzyme reaction; and it establishes the necessary basis of window of operation calculations for targeted optimizations toward different process tasks.

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“…Broad specificity for the nucleophile and low hydrolysis represent a combination of properties that is rare among GHs and makes sucrose phosphorylase a promising transglycosylase candidate, for synthetic applications . The enzyme reaction with glycerol is used industrially to produce the cosmetic ingredient 2-O-α- d -glucosyl glycerol from sucrose (Figure S2 , ). Reactions with l -ascorbic acid and glucose , provide other commercially relevant products, namely, l -ascorbic acid 2-α- d -glucoside and kojibiose, respectively (Figure S2).…”

Section: Introductionmentioning

confidence: 99%

“…The current study was performed to obtain a better understanding of the energetics underlying the versatile catalysis of sucrose phosphorylase. The approach used was a detailed study of temperature effects on steady-state rate parameters for the main types of enzymatic reaction: , phosphorolysis, transglycosylation (to glycerol), and hydrolysis (Figure a).…”

Section: Introductionmentioning

confidence: 99%

Energetics of the Glycosyl Transfer Reactions of Sucrose Phosphorylase

Vyas

Nidetzky

2023

Biochemistry

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From its structure and mechanism, sucrose phosphorylase is a specialized glycoside hydrolase that uses phosphate ions instead of water as the nucleophile of the reaction. Unlike the hydrolysis reaction, the phosphate reaction is readily reversible and, here, this has enabled the study of temperature effects on kinetic parameters to map the energetic profile of the complete catalytic process via a covalent glycosyl enzyme intermediate. Enzyme glycosylation from sucrose and α-glucose 1-phosphate (Glc1P) is rate-limiting in the forward (k cat = 84 s–1) and reverse direction (k cat = 22 s–1) of reaction at 30 °C. Enzyme–substrate association is driven by entropy (TΔS b ≥ +23 kJ/mol), likely arising from enzyme desolvation at the binding site for the leaving group. Approach from the ES complex to the transition state involves uptake of heat (ΔH ⧧ = 72 ± 5.2 kJ/mol) with little further change in entropy. The free energy barrier for the enzyme-catalyzed glycoside bond cleavage in the substrate is much lower than that for the non-enzymatic reaction (k non), ΔΔG ⧧ = ΔG non ⧧ – ΔG enzyme ⧧ = +72 kJ/mol; sucrose. This ΔΔG ⧧, which also describes the virtual binding affinity of the enzyme for the activated substrate in the transition state (∼1014 M–1), is almost entirely enthalpic in origin. The enzymatic rate acceleration (k cat/k non) is ∼1012-fold and similar for reactions of sucrose and Glc1P. The 103-fold lower reactivity (k cat/K m) of glycerol than fructose in enzyme deglycosylation reflects major losses in the activation entropy, suggesting a role of nucleophile/leaving group recognition by the enzyme in inducing the active-site preorganization required for optimum transition state stabilization by enthalpic forces.

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Three‐level hybrid modeling for systematic optimization of biocatalytic synthesis: α‐glucosyl glycerol production by enzymatic trans‐glycosylation from sucrose

Cited by 6 publications

References 65 publications

Pushing the boundaries of phosphorylase cascade reaction for cellobiose production II: Model‐based multiobjective optimization

Pushing the boundaries of phosphorylase cascade reaction for cellobiose production II: Model‐based multiobjective optimization

Pushing the boundaries of phosphorylase cascade reaction for cellobiose production I: Kinetic model development

Energetics of the Glycosyl Transfer Reactions of Sucrose Phosphorylase

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