Glycopeptide-resistant Enterococcus faecium. Analysis of the resistance genotype, virulence and genetic lines [Enterococcus faecium resistente a glucopéptidos. Análisis del genotipo de resistencia, virulencia y líneas genéticas]
- López, M. 1
- Álvarez-Martínez, M.J. 23
- Marco, F. 23
- Torres, C. 1
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1
Universidad de La Rioja
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2
Universitat de Barcelona
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3
Hospital Clinic Barcelona
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ISSN: 0213-005X
Year of publication: 2013
Volume: 31
Issue: 1
Pages: 10-14
Type: Article
beta Ver similares en nube de resultadosMore publications in: Enfermedades Infecciosas y Microbiologia Clinica
Abstract
Objective: The objective of this study was to analyse the genotypic characteristics of all Enterococcus isolates with acquired vancomycin resistance (VRE) recovered in the Hospital Clinic (Barcelona, Spain) in a period of three years and two months. Methods: All VRE isolated in the referred Hospital in the period January 2004-March 2007 were included in the study. The vancomycin resistance mechanism was investigated, as well as other antibiotic resistance mechanisms. Isolates were also typed by pulsed-field-gel-electrophoresis (PFGE) and multi-locus-sequence-typing (MLST). Results: Thirty-nine VRE were recovered, all being identified as E. faecium, representing 2% of total enterococci obtained in that period. Thirty-eight of them carried the vanA gene, and one isolate the vanB2 gene. The 39 VRE were classified into 13 different pulsotypes (A-M), with one main pulsotype, A, which included 13 isolates. The sequence type was identified by MLST in 24 VRE (with unrelated or closely-related PFGE patterns), and they were ascribed to the clonal complex CC17, but two classified as CC9. All VRE showed a multiresistance phenotype, including, in most cases ampicillin, ciprofloxacin, erythromycin, streptomycin, gentamicin, kanamycin and chloramphenicol, harbouring multiple antibiotic resistance genes. The presence of esp and/or hyl genes was identified in 37 VRE. Conclusion: All VRE, but one, showed the vanA genotype and they were mostly ascribed to the high-risk clonal complex CC17. © 2012 Elsevier España, S.L. All rights reserved.