home > bioproject > PRJEB11950
identifier PRJEB11950
type bioproject
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title Multi-drug resistant E.coli strains isolated from dogs at the Edinburgh University Veterinary School as well as A subset of strains associated with community-acquired canine UTI
description Vet Microbiol. 2014 Mar 14;169(3-4):171-8. doi: 10.1016/j.vetmic.2014.01.003. Epub 2014 Jan 13. Multidrug-resistant Escherichia coli from canine urinary tract infections tend to have commensal phylotypes, lower prevalence of virulence determinants and ampC-replicons. Wagner S1, Gally DL1, Argyle SA2. Abstract Multidrug-resistant Escherichia coli is an emerging clinical challenge in domestic species. Treatment options in many cases are limited. This study characterized MDR E. coli isolates from urinary tract infections in dogs, collected between 2002 and 2011. Isolates were evaluated in terms of β-lactamase production, phylogenetic group, ST type, replicon type and virulence marker profile. Comparisons were made with antibiotic susceptible isolates also collected from dogs with urinary tract infections. AmpC β-lactamase was produced in 67% of the MDR isolates (12/18). Of these, 8 could be specifically attributed to the CMY-2 gene. None of the isolates tested in either group expressed ESBLs. Phylo-group distribution was as expected in the susceptible isolates, with an over representation of the pathogenic B2 phylo-group (67%). In contrast, the phylogenetic background for the MDR group was mixed, with representation of commensal phylo-groups A and B1. The B2 phylo-group represented the smallest proportion (A, B1, B2 or D was 28%, 22%, 11% and 33%, respectively). Virulence marker profiles, evaluated using Identibac(®) microarray, discriminated between the two groups. Marker sequences for a core panel of virulence determinants were identified in most of the susceptible isolates, but not in most of the MDR isolates. These findings indicate that for MDR isolates, plasmid-mediated AmpC is an important resistance mechanism, and while still capable of causing clinical disease, there is evidence for a shift towards phylogenetic groups of reduced inferred virulence potential. There was no evidence of zoonotic potential in either the susceptible or MDR urinary tract isolates in this study.
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Multidrug-resistant Escherichia coli from canine urinary tract infections tend to have commensal phylotypes, lower prevalence of virulence determinants and ampC-replicons.
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dbXrefs
sra-run  ERR1148527ERR1148528ERR1148529ERR1148530ERR1148531ERR1148532ERR1148533ERR1148534ERR1148535ERR1148536 More
sra-submission  ERA540622
biosample  SAMEA3681619SAMEA3681620SAMEA3681621SAMEA3681622SAMEA3681623SAMEA3681624SAMEA3681625SAMEA3681626SAMEA3681627SAMEA3681628 More
sra-study  ERP013380
sra-sample  ERS988768ERS988769ERS988770ERS988771ERS988772ERS988773ERS988774ERS988775ERS988776ERS988777 More
sra-experiment  ERX1227531ERX1227532ERX1227533ERX1227534ERX1227535ERX1227536ERX1227537ERX1227538ERX1227539ERX1227540 More
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visibility unrestricted-access
dateCreated 2016-01-31T00:00:00Z
dateModified 2016-01-31T00:00:00Z
datePublished 2016-01-31T00:00:00Z