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Nature AND nurture: enabling formate-dependent growth in Methanosarcina acetivorans

  • UNIVERSITE PARIS CITE
  • Technische Universität Dresden

Tutkimustuotos: LehtiartikkeliArticleScientificvertaisarvioitu

6 Sitaatiot (Scopus)
21 Lataukset (Pure)

Abstrakti

Methanosarcinales are versatile methanogens, capable of regulating most types of methanogenic pathways. Despite the versatile metabolic flexibility of Methanosarcinales, no member of this order has been shown to use formate for methanogenesis. In the present study, we identified a cytosolic formate dehydrogenase (FdhAB) present in several Methanosarcinales, likely acquired by independent horizontal gene transfers after an early evolutionary loss, encouraging re-evaluation of our understanding of formate utilization in Methanosarcinales. To explore whether formate-dependent (methyl-reducing or CO2-reducing) methanogenesis can occur in Methanosarcinales, we engineered two different strains of Methanosarcina acetivorans by functionally expressing FdhAB from Methanosarcina barkeri in M. acetivorans. In the first strain, fdhAB was integrated into the N5-methyl- tetrahydrosarcinapterin:coenzyme M methyltransferase (mtr) operon, making it capable of growing by reducing methanol with electrons from formate. In the second strain, fdhAB was integrated into the F420-reducing hydrogenase (frh) operon, instead of the mtr operon, enabling its growth with formate as the only source of carbon and energy after adaptive laboratory evolution. In this strain, one CO2 is reduced to one methane with electrons from oxidizing four formate to four CO2, a metabolism reported only in methanogens without cytochromes. Although methanogens without cytochromes typically utilize flavin-based electron bifurcation to generate the ferredoxins needed for CO2 activation, we hypothesize that, in our engineered strains, reduced ferredoxins are obtained via the Rhodobacter nitrogen fixation complex complex running in reverse. Our work demonstrates formate-dependent methyl-reducing and CO2-reducing methanogenesis in M. acetivorans that is enabled by the flexible nature of the microbe working in tandem with the nurturing provided.

AlkuperäiskieliEnglanti
Sivut2251-2271
Sivumäärä21
JulkaisuFEBS Journal
Vuosikerta292
Numero9
Varhainen verkossa julkaisun päivämäärä31 tammik. 2025
DOI - pysyväislinkit
TilaJulkaistu - toukok. 2025
OKM-julkaisutyyppiA1 Alkuperäisartikkeli tieteellisessä aikakauslehdessä

Rahoitus

We thank Professor Alfred Spormann, Dr Boyang Ji and Dr Christian Molina for helpful discussions. This research has received financial support from the NovoNordisk foundation (Grant no NNF19OC0054329 to SS and grant no NNF20OC0065032 to JB), the Research Council of Finland (Grant no 329510 to SS), Agence Nationale de la Recherche (Grant no ANR-19-CE02-0005-01 to GB), and the Bundesministerium für Bildung und Forschung (grant no 031B0851A to MR). We thank Professor William Metcalf (University of Illinois, USA), Professor Kyle Costa (University of Minnesota, USA) and Professor Nicole Buan (University of Nebraska-Lincoln, USA) for providing the strains and plasmids used in this study. We also acknowledge the Aalto University Raw Materials Research Infrastructures and Bioeconomy facilities.

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