Literature DB >> 20118248

Functional analysis of the RdxA and RdxB nitroreductases of Campylobacter jejuni reveals that mutations in rdxA confer metronidazole resistance.

Deborah A Ribardo1, Lacey K Bingham-Ramos, David R Hendrixson.   

Abstract

Campylobacter jejuni is a leading cause of gastroenteritis in humans and a commensal bacterium of the intestinal tracts of many wild and agriculturally significant animals. We identified and characterized a locus, which we annotated as rdxAB, encoding two nitroreductases. RdxA was found to be responsible for sensitivity to metronidazole (Mtz), a common therapeutic agent for another epsilonproteobacterium, Helicobacter pylori. Multiple, independently derived mutations in rdxA but not rdxB resulted in resistance to Mtz (Mtz(r)), suggesting that, unlike the case in H. pylori, Mtz(r) might not be a polygenic trait. Similarly, Mtz(r) C. jejuni was isolated after both in vitro and in vivo growth in the absence of selection that contained frameshift, point, insertion, or deletion mutations within rdxA, possibly revealing genetic variability of this trait in C. jejuni due to spontaneous DNA replication errors occurring during normal growth of the bacterium. Similar to previous findings with H. pylori RdxA, biochemical analysis of C. jejuni RdxA showed strong oxidase activity, with reduction of Mtz occurring only under anaerobic conditions. RdxB showed similar characteristics but at levels lower than those for RdxA. Genetic analysis confirmed that rdxA and rdxB are cotranscribed and induced during in vivo growth in the chick intestinal tract, but an absence of these genes did not strongly impair C. jejuni for commensal colonization. Further studies indicate that rdxA is a convenient locus for complementation of mutants in cis. Our work contributes to the growing knowledge of determinants contributing to susceptibility to Mtz (Mtz(s)) and supports previous observations of the fundamental differences in the activities of nitroreductases from epsilonproteobacteria.

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Year:  2010        PMID: 20118248      PMCID: PMC2838047          DOI: 10.1128/JB.01638-09

Source DB:  PubMed          Journal:  J Bacteriol        ISSN: 0021-9193            Impact factor:   3.490


  55 in total

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Review 3.  Treatment of Helicobacter pylori.

Authors:  K Wolle; P Malfertheiner
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5.  Genetic instability is associated with changes in the colonization potential of Campylobacter jejuni in the avian intestine.

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Review 6.  Reduction of polynitroaromatic compounds: the bacterial nitroreductases.

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9.  Characterization of two putative cytochrome c peroxidases of Campylobacter jejuni involved in promoting commensal colonization of poultry.

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10.  Genome dynamics of Campylobacter jejuni in response to bacteriophage predation.

Authors:  Andrew E Scott; Andrew R Timms; Phillippa L Connerton; Catherine Loc Carrillo; Khairul Adzfa Radzum; Ian F Connerton
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Journal:  Gut Microbes       Date:  2012-03-01

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Journal:  FEMS Microbiol Rev       Date:  2016-11-01       Impact factor: 16.408

4.  RNase III-mediated processing of a trans-acting bacterial sRNA and its cis-encoded antagonist.

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Journal:  Elife       Date:  2021-11-29       Impact factor: 8.140

5.  Modulation of Iron Import and Metronidazole Resistance in Bacteroides fragilis Harboring a nimA Gene.

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Journal:  Front Microbiol       Date:  2022-06-09       Impact factor: 6.064

6.  Campylobacter jejuni BumSR directs a response to butyrate via sensor phosphatase activity to impact transcription and colonization.

Authors:  Kyle N Goodman; Matthew J Powers; Alexander A Crofts; M Stephen Trent; David R Hendrixson
Journal:  Proc Natl Acad Sci U S A       Date:  2020-05-12       Impact factor: 11.205

7.  A three-dimensional intestinal tissue model reveals factors and small regulatory RNAs important for colonization with Campylobacter jejuni.

Authors:  Mona Alzheimer; Sarah L Svensson; Fabian König; Matthias Schweinlin; Marco Metzger; Heike Walles; Cynthia M Sharma
Journal:  PLoS Pathog       Date:  2020-02-18       Impact factor: 6.823

  7 in total

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