Engineering the biological conversion of formate into crotonate in Cupriavidus necator

Florent Collas; Beau B Dronsella; Armin Kubis; Karin Schann; Sebastian Binder; Nils Arto; Nico J Claassens; Frank Kensy; Enrico Orsi

doi:10.1016/j.ymben.2023.06.015

Engineering the biological conversion of formate into crotonate in Cupriavidus necator

Metab Eng. 2023 Sep:79:49-65. doi: 10.1016/j.ymben.2023.06.015. Epub 2023 Jul 4.

Authors

Florent Collas¹, Beau B Dronsella², Armin Kubis¹, Karin Schann², Sebastian Binder¹, Nils Arto¹, Nico J Claassens³, Frank Kensy¹, Enrico Orsi⁴

Affiliations

¹ b.fab GmbH, Cologne, Germany.
² Max Planck Institute of Molecular Plant Physiology, Potsdam-Golm, Germany.
³ Laboratory of Microbiology, Wageningen University, Wageningen, the Netherlands.
⁴ Max Planck Institute of Molecular Plant Physiology, Potsdam-Golm, Germany. Electronic address: enricoo@biosustain.dtu.dk.

PMID: 37414134
DOI: 10.1016/j.ymben.2023.06.015

Abstract

To advance the sustainability of the biobased economy, our society needs to develop novel bioprocesses based on truly renewable resources. The C1-molecule formate is increasingly proposed as carbon and energy source for microbial fermentations, as it can be efficiently generated electrochemically from CO₂ and renewable energy. Yet, its biotechnological conversion into value-added compounds has been limited to a handful of examples. In this work, we engineered the natural formatotrophic bacterium C. necator as cell factory to enable biological conversion of formate into crotonate, a platform short-chain unsaturated carboxylic acid of biotechnological relevance. First, we developed a small-scale (150-mL working volume) cultivation setup for growing C. necator in minimal medium using formate as only carbon and energy source. By using a fed-batch strategy with automatic feeding of formic acid, we could increase final biomass concentrations 15-fold compared to batch cultivations in flasks. Then, we engineered a heterologous crotonate pathway in the bacterium via a modular approach, where each pathway section was assessed using multiple candidates. The best performing modules included a malonyl-CoA bypass for increasing the thermodynamic drive towards the intermediate acetoacetyl-CoA and subsequent conversion to crotonyl-CoA through partial reverse β-oxidation. This pathway architecture was then tested for formate-based biosynthesis in our fed-batch setup, resulting in a two-fold higher titer, three-fold higher productivity, and five-fold higher yield compared to the strain not harboring the bypass. Eventually, we reached a maximum product titer of 148.0 ± 6.8 mg/L. Altogether, this work consists in a proof-of-principle integrating bioprocess and metabolic engineering approaches for the biological upgrading of formate into a value-added platform chemical.

Keywords: C1 bioeconomy; Crotonate; Cupriavidus necator; Fed-batch; Formate; Formate toxicity; Modular pathway engineering; Reverse beta-oxidation.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Carbon / metabolism
Crotonates / metabolism
Cupriavidus necator* / genetics
Formates / metabolism
Metabolic Engineering / methods

Substances

formic acid
Crotonates
Formates
Carbon