4.7 Article

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

Journal

METABOLIC ENGINEERING
Volume 73, Issue -, Pages 256-269

Publisher

ACADEMIC PRESS INC ELSEVIER SCIENCE
DOI: 10.1016/j.ymben.2022.08.005

Keywords

Cupriavidus necator; Metabolic versatility; Metabolic modeling; Thermodynamics; PHB; Elementary flux modes; Formatotrophy

Funding

  1. Swedish Research Council Vetenskapsradet [2016-06160]
  2. Novo Nordisk Fonden [NNF20OC0061469]
  3. Swedish Research Council Formas [2016-20006]
  4. Swedish Research Council [2016-06160] Funding Source: Swedish Research Council
  5. Formas [2016-20006] Funding Source: Formas

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This study analyzed the thermodynamic driving forces and PHB yields of the chemolithotroph Cupriavidus necator H16 from formate using different metabolic engineering strategies. Heterologous reactions were predicted and verified experimentally to increase driving force and PHB production. The findings provide insights into metabolic adaptation and can be applied in designing metabolic engineering strategies for other non-model bacteria.
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 from formate for 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 then verified experimentally to enhance PHB titers between 60 and 300% in select conditions. The EFM analysis also revealed that PHB production from formate may be limited by low driving forces through citrate lyase and aconitase, as well as cofactor balancing, and identified additional reactions associated with low and high PHB yield. Proteomics analysis of the engineered strains confirmed an increased abundance of aconitase and cofactor balancing. The findings of this study aid in understanding metabolic adaptation. Furthermore, the outlined approach will be useful in designing metabolic engineering strategies in other non-model bacteria.

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