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Overcoming genetic heterogeneity in industrial fermentations.

Peter RugbjergMorten Otto Alexander Sommer
Published in: Nature biotechnology (2019)
Engineering the synthesis of massive amounts of therapeutics, enzymes or commodity chemicals can select for subpopulations of nonproducer cells, owing to metabolic burden and product toxicity. Deep DNA sequencing can be used to detect undesirable genetic heterogeneity in producer populations and diagnose associated genetic error modes. Hotspots of genetic heterogeneity can pinpoint mechanisms that underlie load problems and product toxicity. Understanding genetic heterogeneity will inform metabolic engineering and synthetic biology strategies to minimize the emergence of nonproducer mutants in scaled-up fermentations and maximize product quality and yield.
Keyphrases
  • single cell
  • genome wide
  • copy number
  • oxidative stress
  • mental health
  • small molecule
  • wastewater treatment
  • saccharomyces cerevisiae
  • single molecule
  • cell free
  • cell death
  • cell cycle arrest