Programming Saposin-Mediated Compensatory Metabolic Sinks for Enhanced Ubiquinone Production

  • Wen Xu
  • , Jifeng Yuan
  • , Shuiyun Yang
  • , Chi Bun Ching
  • , Jiankang Liu

Research output: Contribution to journalArticlepeer-review

13 Scopus citations

Abstract

Microbial synthesis of ubiquinone by fermentation processes has been emerging in recent years. However, as ubiquinone is a primary metabolite that is tightly regulated by the host central metabolism, tweaking the individual pathway components could only result in a marginal improvement on the ubiquinone production. Given that ubiquinone is stored in the lipid bilayer, we hypothesized that introducing additional metabolic sink for storing ubiquinone might improve the CoQ10 production. As human lipid binding/transfer protein saposin B (hSapB) was reported to extract ubiquinone from the lipid bilayer and form the water-soluble complex, hSapB was chosen to build a compensatory metabolic sink for the ubiquinone storage. As a proof-of-concept, hSapB-mediated metabolic sink systems were devised and systematically investigated in the model organism of Escherichia coli. The hSapB-mediated periplasmic sink resulted in more than 200% improvement of CoQ8 over the wild type strain. Further investigation revealed that hSapB-mediated sink systems could also improve the CoQ10 production in a CoQ10-hyperproducing E. coli strain obtained by a modular pathway rewiring approach. As the design principles and the engineering strategies reported here are generalizable to other microbes, compensatory sink systems will be a method of significant interest to the synthetic biology community.

Original languageEnglish
Pages (from-to)1404-1411
Number of pages8
JournalACS Synthetic Biology
Volume5
Issue number12
DOIs
StatePublished - 16 Dec 2016

Keywords

  • metabolic sink
  • modular pathway rewiring
  • saposin
  • synthetic biology
  • ubiquinone-binding protein

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