Abstract

BackgroundLipids are important precursors in the biofuel and oleochemical industries. Yarrowia lipolytica is among the most extensively studied oleaginous microorganisms and has been a focus of metabolic engineering to improve lipid production. Yield improvement, through rewiring of the central carbon metabolism of Y. lipolytica from glucose to the lipid precursor acetyl-CoA, is a key strategy for achieving commercial success in this organism.ResultsBuilding on YB-392, a Y. lipolytica isolate known for stable non-hyphal growth and low citrate production with demonstrated potential for high lipid accumulation, we assembled a heterologous pathway that redirects carbon flux from glucose through the pentose phosphate pathway (PPP) to acetyl-CoA. We used phosphofructokinase (Pfk) deletion to block glycolysis and expressed two non-native enzymes, phosphoketolase (Xpk) and phosphotransacetylase (Pta), to convert PPP-produced xylulose-5-P to acetyl-CoA. Introduction of the pathway in a pfk deletion strain that is unable to grow and accumulate lipid from glucose in defined media ensured maximal redirection of carbon flux through Xpk/Pta. Expression of Xpk and Pta restored growth and lipid production from glucose. In 1-L bioreactors, the engineered strains recorded improved lipid yield and cell-specific productivity by up to 19 and 78%, respectively.ConclusionsYields and cell-specific productivities are important bioprocess parameters for large-scale lipid fermentations. Improving these parameters by engineering the Xpk/Pta pathway is an important step towards developing Y. lipolytica as an industrially preferred microbial biocatalyst for lipid production.

Highlights

  • Lipids are important precursors in the biofuel and oleochemical industries

  • Identification of functional heterologous phosphotransacetylase (PTA) and phosphoketolase (XPK) in Y. lipolytica Heterologous PTA and XPK genes from various species of bacteria, archaea, algae and fungi were tested for activity in Y. lipolytica

  • Genes were individually expressed in wild-type strain YB-392 and cell-free extracts were assayed to measure Pta and Xpk activity

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Summary

Introduction

Lipids are important precursors in the biofuel and oleochemical industries. Yarrowia lipolytica is among the most extensively studied oleaginous microorganisms and has been a focus of metabolic engineering to improve lipid production. Through rewiring of the central carbon metabolism of Y. lipolytica from glucose to the lipid precursor acetyl-CoA, is a key strategy for achieving commercial success in this organism. Yarrowia lipolytica has emerged as the preferred organism to study and engineer lipid production [6]. It is an oleaginous yeast capable of accumulating. Lipid composition alterations to make industrially relevant products like triolein have been demonstrated in Y. lipolytica [12]. Y. lipolytica is often chosen as a model organism to study the glucose-to-lipid pathway, lipid body biogenesis and homeostasis [4, 13, 14]

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