Literature DB >> 26810657

Fumarate-Mediated Persistence of Escherichia coli against Antibiotics.

Jun-Seob Kim1, Da-Hyeong Cho2, Paul Heo2, Suk-Chae Jung2, Myungseo Park2, Eun-Joong Oh3, Jaeyun Sung4, Pan-Jun Kim5, Suk-Chan Lee2, Dae-Hee Lee6, Sarah Lee7, Choong Hwan Lee7, Dongwoo Shin8, Yong-Su Jin9, Dae-Hyuk Kweon10.   

Abstract

Bacterial persisters are a small fraction of quiescent cells that survive in the presence of lethal concentrations of antibiotics. They can regrow to give rise to a new population that has the same vulnerability to the antibiotics as did the parental population. Although formation of bacterial persisters in the presence of various antibiotics has been documented, the molecular mechanisms by which these persisters tolerate the antibiotics are still controversial. We found that amplification of the fumarate reductase operon (FRD) inEscherichia coliled to a higher frequency of persister formation. The persister frequency ofE. coliwas increased when the cells contained elevated levels of intracellular fumarate. Genetic perturbations of the electron transport chain (ETC), a metabolite supplementation assay, and even the toxin-antitoxin-relatedhipA7mutation indicated that surplus fumarate markedly elevated theE. colipersister frequency. AnE. colistrain lacking succinate dehydrogenase (SDH), thereby showing a lower intracellular fumarate concentration, was killed ∼1,000-fold more effectively than the wild-type strain in the stationary phase. It appears thatSDHandFRDrepresent a paired system that gives rise to and maintainsE. colipersisters by producing and utilizing fumarate, respectively.
Copyright © 2016, American Society for Microbiology. All Rights Reserved.

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Year:  2016        PMID: 26810657      PMCID: PMC4808198          DOI: 10.1128/AAC.01794-15

Source DB:  PubMed          Journal:  Antimicrob Agents Chemother        ISSN: 0066-4804            Impact factor:   5.191


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