Extension of the hydrolysis spectrum of AmpC {beta}-lactamase of Escherichia coli due to amino acid insertion in the H-10 helix

doi:10.1093/jac/dkm227

JAC Advance Access originally published online on June 22, 2007
Journal of Antimicrobial Chemotherapy 2007 60(3):490-494; doi:10.1093/jac/dkm227

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© The Author 2007. Published by Oxford University Press on behalf of the British Society for Antimicrobial Chemotherapy. All rights reserved. For Permissions, please e-mail: journals.permissions@oxfordjournals.org

Extension of the hydrolysis spectrum of AmpC ß-lactamase of Escherichia coli due to amino acid insertion in the H-10 helix

Hedi Mammeri, Laurent Poirel and Patrice Nordmann^*

Service de Bactériologie-Virologie, Hôpital de Bicêtre, Assistance Publique/Hôpitaux de Paris, Faculté de Médecine Paris-Sud, Université Paris Sud, 94275 K.-Bicêtre, France

Received 28 December 2006; returned 22 February 2007; revised 2 May 2007; accepted 30 May 2007

^* Corresponding author. Tel: +33-1-45-21-36-32; Fax: +33-1-45-21-63-40; E-mail: nordmann.patrice{at}bct.aphp.fr

Objectives: To characterize the naturally occurring expanded-spectrum ß-lactamasefrom an Escherichia coli clinical isolate and to compare itwith a wild-type ß-lactamase.

Methods: The chromosome-borne ampC genes from E. coli BER and E. coliEC2 were PCR amplified, sequenced and cloned into an expressionvector. Antimicrobial susceptibilities of the parental isolateand the recombinant strains were determined by agar dilutionmethods. Kinetic parameters were determined from purified AmpCBER and AmpC EC2.

Results: AmpC BER was overexpressed in its original clinical isolatebecause of mutations in the promoter region of its gene at positions–42 and –18. The analysis of the ampC coding sequencerevealed a 6 bp insertion when compared with the wild-type sequenceleading to the tandem duplication of two alanine residues insidethe H-10 helix. AmpC BER-producing recombinants were resistantto ceftazidime, had reduced susceptibility to other oxyiminocephalosporins(cefotaxime and cefepime), but had a greater susceptibilityto cefoxitin when compared with the recombinant expressing thewild-type ß-lactamase AmpC EC2. The affinity of AmpCBER for cephalosporins and imipenem was increased, whereas thehydrolysis rate was decreased for all these compounds. In addition,the IC₅₀ values of clavulanic acid and tazobactam for AmpC BERwere increased.

Conclusions: This work sheds new light on structure–function relationshipsof expanded-spectrum AmpC ß-lactamases.

Keywords: expanded-spectrum AmpC , cefepime , E. coli

Present address. Service de Bactériologie-Hygiène,Centre Hospitalier Universitaire d'Amiens, Hôpital, Nord,2 Place Victor Pauchet, 80080 Amiens, France.

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