Protein allocation and utilization in the versatile chemolithoautotroph<i>Cupriavidus necator</i>

Jahn, Michael; Crang, Nick; Janasch, Markus; Hober, Andreas; Kimler, Kyle; Mattausch, Alexander; Chen, Qi; Asplund-Samuelsson, Johannes; Hudson, Elton P.

doi:10.1101/2021.03.21.436304

Cited by 2 publications

(8 citation statements)

References 64 publications

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“…For each EFM we determined the biomass yield, the PHB yield, and the MDF value (Figure 2A-B, Figure S3). While the maximum biomass yield observed for formate (∼0.12 g biomass /g substrate ) corresponded well to experimental results (Grunwald et al, 2015; Jahn et al, 2021), the model overestimated the maximum biomass yield for fructose (∼0.53 g biomass /g substrate , Figure 2A). In vivo flux distributions on this substrate are therefore likely to contain EFMs with lower yields.…”

Section: Resultssupporting

confidence: 84%

“…This apparent disagreement arises because the addition of Xfpk allows both high and lower-yield EFMs, so its yield score is not high. On fructose, a functional CBB cycle, represented by PRK and RUBISCO, had a negative score for biomass yield, which agrees with yields determined by proteomics-constrained flux simulations (Jahn et al, 2021). The CBB cycle requires ATP and NADPH, whose production requires decarboxylation in lower glycolysis and the TCA cycle, diverting carbon away from biomass.…”

Section: Resultssupporting

confidence: 79%

“…Common reactions with high DFs in the two metabolic strategies were found in the anaplerotic reactions (MAE, PEPC), as well as some CBB cycle reactions (RUBISCO, PRK, GADPH, FBA, FBPase, SBPase), implying lower expression levels to carry flux. However, having a high DF is no guarantee of low expression levels, as is exemplified by the high protein levels of RUBISCO, an enzyme limited by its low rate (Jahn et al, 2021). While it is challenging to precisely determine which metabolic strategy (or combination of EFMs) is used for PHB production in vivo based on stoichiometry and thermodynamics alone, essentiality analysis, such as through use of genetic knockout libraries (Jahn et al, 2021), could help to elucidate the actual in vivo flux distribution to PHB.…”

Section: Resultsmentioning

confidence: 99%

“…Which EFMs are preferentially used in vivo could be better predicted with additional physiological constraints on the solution space, such as protein abundance, gene essentiality, and enzyme kinetics and biochemical regulations (Gerosa et al, 2015; Jahn et al, 2021; Sánchez et al, 2017). Along those lines, a transposon-library of C. necator identified ACS and PEPC as essential reactions, hinting towards their usage in vivo (Jahn et al, 2021).…”

Section: Resultsmentioning

confidence: 99%

“…The color of each EFM corresponds to its MDF value. White diamonds indicate measured yields from chemostat experiments of the H16 wild-type at different dilution rates, taken from (Jahn et al, 2021). B) Same as A) but for formate.…”

Section: Model and Methodsmentioning

confidence: 99%

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Thermodynamic limitations of metabolic strategies for PHB production from formate and fructose in Cupriavidus necator

Janasch

Crang

Bruch

et al. 2022

Preprint

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The chemolithotroph Cupriavidus necator H16 is known as a natural producer of the bioplastic-polymer PHB, as well as for its metabolic versatility to utilize different substrates, including formate as the sole carbon and energy source. Depending on the entry point of the substrate, this versatility requires adjustment of the thermodynamic landscape to maintain sufficiently high driving forces for biological processes. Here we employed a model of the core metabolism of C. necator H16 to analyze the thermodynamic driving forces and PHB yields of different metabolic engineering strategies. For this, we enumerated elementary flux modes (EFMs) of the network and evaluated their PHB yields as well as thermodynamics via Max-min driving force (MDF) analysis and random sampling of driving forces. A heterologous ATP:citrate lyase reaction was predicted to increase driving force for producing acetyl-CoA. A heterologous phosphoketolase reaction was predicted to increase maximal PHB yields as well as driving forces. These enzymes were verified experimentally to enhance PHB titers between 60 and 300% in select conditions. The EFM analysis also revealed that metabolic strategies for PHB production from formate may be limited by low driving forces through citrate lyase and aconitase, as well as cofactor balancing, and identified reactions of the core metabolism associated with low and high PHB yield. The findings of this study aid in understanding metabolic adaptation. Furthemore, the outlined approach will be useful in designing metabolic engineering strategies in other non-model bacteria.

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Section: Resultssupporting

confidence: 84%

Section: Resultssupporting

confidence: 79%

Section: Resultsmentioning

confidence: 99%

Section: Resultsmentioning

confidence: 99%

Section: Model and Methodsmentioning

confidence: 99%

See 3 more Smart Citations

Thermodynamic limitations of metabolic strategies for PHB production from formate and fructose in Cupriavidus necator

Janasch

Crang

Bruch

et al. 2022

Preprint

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Metabolite interactions in the bacterial Calvin cycle and implications for flux regulation

Sporre

Karlsen

Schriever

et al. 2022

Preprint

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Metabolite-level regulation of enzyme activity is important for coping with environmental shifts in bacteria. Improved understanding of such regulation could guide attempts to engineer more efficient strains for biochemical production. Recently developed proteomics methods allow for mapping of post-translational interactions, including metabolite-protein interactions, that may be relevant for quickly regulating pathway activity. While feed-back and feed-forward regulation in glycolysis has been investigated, there is relatively little study of metabolite-level regulation in the Calvin cycle, particularly in bacteria. Here, we applied limited proteolysis small molecule mapping (LiP-SMap) to identify and compare metabolite-protein interactions in four potential metabolic engineering host that fix CO2 using the Calvin cycle, including two photoautotrophs (cyanobacteria) and two chemoautotrophs. Species-specific interactions were observed, such as interactions with glucose-6-phosphate in the chemoautotroph Cupriavidus necator and interactions with glyoxylate in the cyanobacteria Synechocystis sp. PCC 6803, which suggests that metabolite-level regulation could be adapted to a certain metabolic capacity or lifestyle of these bacteria. Identified metabolite interactions with Calvin cycle enzymes fructose-1,6/sedoheptulose-1,7-bisphosphatase (F/SBPase) and transketolase were tested for effects on catalytic activity using kinetic assays. GAP increased the activity of both Synechocystis and Cupriavidus F/SBPase, which may act as a feed-forward activation mechanism in the Calvin cycle. A kinetic model incorporating regulations on F/SBPase generally enhanced flux control of ATP and NADPH supply over the cycle. We show that LiP-SMap is a promising technique to explore and uncover novel post-translational metabolic regulation, although the method could benefit from improved sensitivity and specificity.

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Protein allocation and utilization in the versatile chemolithoautotrophCupriavidus necator

Cited by 2 publications

References 64 publications

Thermodynamic limitations of metabolic strategies for PHB production from formate and fructose in Cupriavidus necator

Thermodynamic limitations of metabolic strategies for PHB production from formate and fructose in Cupriavidus necator

Metabolite interactions in the bacterial Calvin cycle and implications for flux regulation

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