Literature DB >> 22096151

Escherichia coli enterobactin synthesis and uptake mutants are hypersensitive to an antimicrobial peptide that limits the availability of iron in addition to blocking Holliday junction resolution.

Samantha S Orchard1, Jason E Rostron, Anca M Segall.   

Abstract

The peptide wrwycr inhibits Holliday junction resolution and is a potent antimicrobial. To study the physiological effects of wrwycr treatment on Escherichia coli cells, we partially screened the Keio collection of knockout mutants for those with increased sensitivity to wrwycr. Strains lacking part of the ferric-enterobactin (iron-bound siderophore) uptake and utilization system, parts of the enterobactin synthesis pathway, TolC (an outer-membrane channel protein) or Fur (an iron-responsive regulator) were hypersensitive to wrwycr. We provide evidence that the ΔtolC mutant was hypersensitive to wrwycr due to its reduced ability to efflux wrwycr from the cell rather than due to its export of newly synthesized enterobactin. Deleting ryhB, which encodes a small RNA involved in iron regulation, mostly relieved the wrwycr hypersensitivity of the fur and ferric-enterobactin uptake mutants, indicating that the altered regulation of a RyhB-controlled gene was at least partly responsible for the hypersensitivity of these strains. Chelatable iron in the cell, measured by electron paramagnetic resonance spectroscopy, increased dramatically following wrwycr treatment, as did expression of Fur-repressed genes and, to some extent, mutation frequency. These incongruous results suggest that while wrwycr treatment caused accumulation of chelatable iron in the cell, iron was not available to bind to Fur. This is corroborated by the observed induction of the suf system, which assembles iron-sulfur clusters in low-iron conditions. Disruption of iron metabolism by wrwycr, in addition to its effects on DNA repair, may make it a particularly effective antimicrobial in the context of the low-iron environment of a mammalian host.

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Year:  2011        PMID: 22096151      PMCID: PMC3352285          DOI: 10.1099/mic.0.054361-0

Source DB:  PubMed          Journal:  Microbiology        ISSN: 1350-0872            Impact factor:   2.777


  45 in total

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5.  The neutrophil lipocalin NGAL is a bacteriostatic agent that interferes with siderophore-mediated iron acquisition.

Authors:  David H Goetz; Margaret A Holmes; Niels Borregaard; Martin E Bluhm; Kenneth N Raymond; Roland K Strong
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7.  Intracellular cyclic AMP concentration is decreased in Salmonella typhimurium fur mutants.

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Review 8.  Enterobactin: an archetype for microbial iron transport.

Authors:  Kenneth N Raymond; Emily A Dertz; Sanggoo S Kim
Journal:  Proc Natl Acad Sci U S A       Date:  2003-03-24       Impact factor: 11.205

9.  Export of the siderophore enterobactin in Escherichia coli: involvement of a 43 kDa membrane exporter.

Authors:  Jason L Furrer; Douglas N Sanders; India G Hook-Barnard; Mark A McIntosh
Journal:  Mol Microbiol       Date:  2002-06       Impact factor: 3.501

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Authors:  Eric Massé; Freddy E Escorcia; Susan Gottesman
Journal:  Genes Dev       Date:  2003-09-15       Impact factor: 12.890

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  7 in total

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2.  wrwyrggrywrw is a single-chain functional analog of the Holliday junction-binding homodimer, (wrwycr)2.

Authors:  Marc C Rideout; Ilham Naili; Jeffrey L Boldt; America Flores-Fujimoto; Sukanya Patra; Jason E Rostron; Anca M Segall
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4.  Dps Protects Enterohemorrhagic Escherichia coli against Acid-Induced Antimicrobial Peptide Killing.

Authors:  Tracy Lackraj; Sarah Birstonas; Michele Kacori; Debora Barnett Foster
Journal:  J Bacteriol       Date:  2020-05-11       Impact factor: 3.490

5.  Potentiation of Antibiotics by a Novel Antimicrobial Peptide against Shiga Toxin Producing E. coli O157:H7.

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6.  Similarities between exogenously- and endogenously-induced envelope stress: the effects of a new antibacterial molecule, TPI1609-10.

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7.  Quantitative genome-wide genetic interaction screens reveal global epistatic relationships of protein complexes in Escherichia coli.

Authors:  Mohan Babu; Roland Arnold; Cedoljub Bundalovic-Torma; Alla Gagarinova; Keith S Wong; Ashwani Kumar; Geordie Stewart; Bahram Samanfar; Hiroyuki Aoki; Omar Wagih; James Vlasblom; Sadhna Phanse; Krunal Lad; Angela Yeou Hsiung Yu; Christopher Graham; Ke Jin; Eric Brown; Ashkan Golshani; Philip Kim; Gabriel Moreno-Hagelsieb; Jack Greenblatt; Walid A Houry; John Parkinson; Andrew Emili
Journal:  PLoS Genet       Date:  2014-02-20       Impact factor: 5.917

  7 in total

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