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Functional replacement of isoprenoid pathways in Rhodobacter sphaeroides
Authors:Enrico Orsi  Jules Beekwilder  Dewi van Gelder  Adèle van Houwelingen  Gerrit Eggink  Servé W.M. Kengen  Ruud A. Weusthuis
Affiliation:1. Bioprocess Engineering, Wageningen University, 6708PB Wageningen, The Netherlands;2. Wageningen Plant Research, 6700AA Wageningen, The Netherlands;3. Bioprocess Engineering, Wageningen University, 6708PB Wageningen, The Netherlands

Wageningen Food and Biobased Research, 6708WG Wageningen, The Netherlands;4. Laboratory of Microbiology, Wageningen University, 6708WE Wageningen, The Netherlands

Abstract:Advances in synthetic biology and metabolic engineering have proven the potential of introducing metabolic by-passes within cell factories. These pathways can provide a more efficient alternative to endogenous counterparts due to their insensitivity to host's regulatory mechanisms. In this work, we replaced the endogenous essential 2-C-methyl-D-erythritol 4-phosphate (MEP) pathway for isoprenoid biosynthesis in the industrially relevant bacterium Rhodobacter sphaeroides by an orthogonal metabolic route. The native 2-C-methyl-D-erythritol 4-phosphate (MEP) pathway was successfully replaced by a heterologous mevalonate (MVA) pathway from a related bacterium. The functional replacement was confirmed by analysis of the reporter molecule amorpha-4,11-diene after cultivation with [4-13C]glucose. The engineered R. sphaeroides strain relying exclusively on the MVA pathway was completely functional in conditions for sesquiterpene production and, upon increased expression of the MVA enzymes, it reached even higher sesquiterpene yields than the control strain coexpressing both MEP and MVA modules. This work represents an example where substitution of an essential biochemical pathway by an alternative, heterologous pathway leads to enhanced biosynthetic performance.
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