| Literature DB >> 29530749 |
Kevin W George1, Mitchell G Thompson2, Joonhoon Kim3, Edward E K Baidoo1, George Wang1, Veronica Teixeira Benites1, Christopher J Petzold1, Leanne Jade G Chan1, Suzan Yilmaz1, Petri Turhanen4, Paul D Adams5, Jay D Keasling6, Taek Soon Lee7.
Abstract
Isopentenyl pyrophosphate (IPP) toxicity presents a challenge in engineered microbial systems since its formation is unavoidable in terpene biosynthesis. In this work, we develop an experimental platform to study IPP toxicity in isoprenol-producing Escherichia coli. We first characterize the physiological response to IPP accumulation, demonstrating that elevated IPP levels are linked to growth inhibition, reduced cell viability, and plasmid instability. We show that IPP toxicity selects for pathway "breakage", using proteomics to identify a reduction in phosphomevalonate kinase (PMK) as a probable recovery mechanism. Next, using multi-omics data, we demonstrate that endogenous E. coli metabolism is globally impacted by IPP accumulation, which slows nutrient uptake, decreases ATP levels, and perturbs nucleotide metabolism. We also observe the extracellular accumulation of IPP and present preliminary evidence that IPP can be transported by E. coli, findings that might be broadly relevant for the study of isoprenoid biosynthesis. Finally, we discover that IPP accumulation leads to the formation of ApppI, a nucleotide analog of IPP that may contribute to observed toxicity phenotypes. This comprehensive assessment of IPP stress suggests potential strategies for the alleviation of prenyl diphosphate toxicity and highlights possible engineering targets for improved IPP flux and high titer isoprenoid production.Entities:
Keywords: ApppI; IPP toxicity; Isopentenyl pyrophosphate (IPP); Isoprenol; Mevalonate pathway; Multi-omics
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Year: 2018 PMID: 29530749 DOI: 10.1016/j.ymben.2018.03.004
Source DB: PubMed Journal: Metab Eng ISSN: 1096-7176 Impact factor: 9.783