| Literature DB >> 28527885 |
Kaspar Valgepea1, Renato de Souza Pinto Lemgruber1, Kieran Meaghan1, Robin William Palfreyman1, Tanus Abdalla2, Björn Daniel Heijstra2, James Bruce Behrendorff2, Ryan Tappel2, Michael Köpke2, Séan Dennis Simpson2, Lars Keld Nielsen1, Esteban Marcellin3.
Abstract
Acetogens are promising cell factories for producing fuels and chemicals from waste feedstocks via gas fermentation, but quantitative characterization of carbon, energy, and redox metabolism is required to guide their rational metabolic engineering. Here, we explore acetogen gas fermentation using physiological, metabolomics, and transcriptomics data for Clostridium autoethanogenum steady-state chemostat cultures grown on syngas at various gas-liquid mass transfer rates. We observe that C. autoethanogenum shifts from acetate to ethanol production to maintain ATP homeostasis at higher biomass concentrations but reaches a limit at a molar acetate/ethanol ratio of ∼1. This regulatory mechanism eventually leads to depletion of the intracellular acetyl-CoA pool and collapse of metabolism. We accurately predict growth phenotypes using a genome-scale metabolic model. Modeling revealed that the methylene-THF reductase reaction was ferredoxin reducing. This work provides a reference dataset to advance the understanding and engineering of arguably the first carbon fixation pathway on Earth.Entities:
Keywords: Clostridium autoethanogenum; RNA sequencing; acetogen metabolism; gas fermentation; genome-scale model; intracellular metabolomics; modeling; syngas fermentation; systems biology
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Year: 2017 PMID: 28527885 DOI: 10.1016/j.cels.2017.04.008
Source DB: PubMed Journal: Cell Syst ISSN: 2405-4712 Impact factor: 10.304