4.7 Article

Critical Roles of the Pentose Phosphate Pathway and GLN3 in Isobutanol-Specific Tolerance in Yeast

Journal

CELL SYSTEMS
Volume 9, Issue 6, Pages 534-+

Publisher

CELL PRESS
DOI: 10.1016/j.cels.2019.10.006

Keywords

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Funding

  1. US Department of Energy, Office of Science, Office of Biological and Environmental Research, Genomic Science Program [DESC0019363]
  2. NSF CAREER award [1751840]
  3. Pew Charitable Trusts
  4. Alfred P. Sloan Foundation
  5. Yang Family Foundation for Engineering from Princeton University SEAS
  6. John Mung Program Kyoto University
  7. NSF [DGE-1656466]
  8. NIH [GM035010]
  9. DOE [6935036]
  10. SPIRITS 2017 of Kyoto University
  11. Div Of Chem, Bioeng, Env, & Transp Sys
  12. Directorate For Engineering [1751840] Funding Source: National Science Foundation

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Branched-chain alcohols are attractive advanced biofuels; however, their cellular toxicity is an obstacle to engineering microbes to produce them at high titers. We performed genome- wide screens on the Saccharomyces cerevisiae gene deletion library to identify cell systems involved in isobutanol-specific tolerance. Deletion of pentose phosphate pathway genes GND1 or ZWF1 causes hypersensitivity to isobutanol but not to ethanol. By contrast, deletion of GLN3 increases yeast tolerance specifically to branched-chain alcohols. Transcriptomic analyses revealed that isobutanol induces a nitrogen starvation response via GLN3 and GCN4, upregulating amino acid biosynthesis and nitrogen scavenging while downregulating glycolysis, cell wall biogenesis, and membrane lipid biosynthesis. Disruption of this response by deleting GLN3 is enough to enhance tolerance and boost isobutanol production 4.9-fold in engineered strains. This study illustrates how adaptive mechanisms to tolerate stress can lead to toxicity in microbial fermentations for chemical production and how genetic interventions can boost production by evading such mechanisms.

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