CMY-42, a Novel Plasmid-Mediated CMY-2 Variant AmpC Beta-Lactamase

CMY-42, a Novel Plasmid-Mediated CMY-2 Variant AmpC Beta-Lactamase

We isolated a clinical Escherichia coli strain with an antimicrobial resistance phenotype characteristic for the expression of an AmpC beta-lactamase. Molecular methods revealed a novel, plasmid-localized variant of CMY-2 with a substitution of valine 231 for serine (V231S), which was designated CMY...

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Veröffentlicht in:Microbial drug resistance (Larchmont, N.Y.) N.Y.), 2011-06, Vol.17 (2), p.165-169
Hauptverfasser: Hentschke, Moritz, Kotsakis, Stathis D., Wolters, Manuel, Heisig, Peter, Miriagou, Vivi, Aepfelbacher, Martin
Format: Artikel
Sprache:eng
Schlagworte:
Anti-Bacterial Agents - pharmacology
Antibiotics
Bacteriology
Beta lactamases
beta-Lactamases - genetics
beta-Lactamases - metabolism
Cephalosporins
Cephalosporins - pharmacology
Drug resistance
Drug resistance in microorganisms
Drug Resistance, Bacterial - drug effects
Drug Resistance, Bacterial - genetics
E coli
Escherichia coli
Escherichia coli - genetics
Escherichia coli - growth & development
Escherichia coli - isolation & purification
Escherichia coli Infections - drug therapy
Escherichia coli Infections - genetics
Escherichia coli Infections - microbiology
Escherichia coli Proteins - genetics
Escherichia coli Proteins - metabolism
Genes
Genetic aspects
Genetic susceptibility
Health aspects
Humans
Identification and classification
Mechanisms
Molecular Sequence Data
Plasmids - genetics
Plasmids - metabolism
Serine
Serine - genetics
Serine - metabolism
Surgical Wound Infection - drug therapy
Surgical Wound Infection - genetics
Surgical Wound Infection - microbiology
valine
Valine - genetics
Valine - metabolism
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Zusammenfassung:We isolated a clinical Escherichia coli strain with an antimicrobial resistance phenotype characteristic for the expression of an AmpC beta-lactamase. Molecular methods revealed a novel, plasmid-localized variant of CMY-2 with a substitution of valine 231 for serine (V231S), which was designated CMY-42. Like the CMY-2-like AmpC beta-lactamase CMY-30, carrying the substitution V231G, CMY-42 displayed increased activity toward expanded spectrum cephalosporins. This finding supports the hypothesis that a bulky side chain at position 231 (Ambler's position 211) may pose a steric clash with certain cephalosporins hindering the access of the AmpC beta-lactamase; however, additional phenomena may account for the observed hydrolytic properties.
ISSN:1076-6294
1931-8448
DOI:10.1089/mdr.2010.0137