Literature DB >> 24727267

Evolved osmotolerant Escherichia coli mutants frequently exhibit defective N-acetylglucosamine catabolism and point mutations in cell shape-regulating protein MreB.

James D Winkler1, Carlos Garcia2, Michelle Olson1, Emily Callaway3, Katy C Kao4.   

Abstract

Biocatalyst robustness toward stresses imposed during fermentation is important for efficient bio-based production. Osmotic stress, imposed by high osmolyte concentrations or dense populations, can significantly impact growth and productivity. In order to better understand the osmotic stress tolerance phenotype, we evolved sexual (capable of in situ DNA exchange) and asexual Escherichia coli strains under sodium chloride (NaCl) stress. All isolates had significantly improved growth under selection and could grow in up to 0.80 M (47 g/liter) NaCl, a concentration that completely inhibits the growth of the unevolved parental strains. Whole genome resequencing revealed frequent mutations in genes controlling N-acetylglucosamine catabolism (nagC, nagA), cell shape (mrdA, mreB), osmoprotectant uptake (proV), and motility (fimA). Possible epistatic interactions between nagC, nagA, fimA, and proV deletions were also detected when reconstructed as defined mutations. Biofilm formation under osmotic stress was found to be decreased in most mutant isolates, coupled with perturbations in indole secretion. Transcriptional analysis also revealed significant changes in ompACGL porin expression and increased transcription of sulfonate uptake systems in the evolved mutants. These findings expand our current knowledge of the osmotic stress phenotype and will be useful for the rational engineering of osmotic tolerance into industrial strains in the future.
Copyright © 2014, American Society for Microbiology. All Rights Reserved.

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Year:  2014        PMID: 24727267      PMCID: PMC4054140          DOI: 10.1128/AEM.00499-14

Source DB:  PubMed          Journal:  Appl Environ Microbiol        ISSN: 0099-2240            Impact factor:   4.792


  51 in total

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5.  Evolution combined with genomic study elucidates genetic bases of isobutanol tolerance in Escherichia coli.

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Review 7.  Indole as an intercellular signal in microbial communities.

Authors:  Jin-Hyung Lee; Jintae Lee
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8.  Evolution, genomic analysis, and reconstruction of isobutanol tolerance in Escherichia coli.

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9.  Transcriptional analysis of Lactobacillus brevis to N-butanol and ferulic acid stress responses.

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Review 3.  The emergence of adaptive laboratory evolution as an efficient tool for biological discovery and industrial biotechnology.

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5.  In Vivo Titration of Folate Pathway Enzymes.

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6.  Combinatorial strategies for improving multiple-stress resistance in industrially relevant Escherichia coli strains.

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7.  Adaptive Strategies of the Candidate Probiotic E. coli Nissle in the Mammalian Gut.

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10.  Thermodynamically optimal whole-genome tiling microarray design and validation.

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