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Increased Antimicrobial Resistance in a Novel CMY-54 AmpC-Type Enzyme with a GluLeu Insertion in the Ω-Loop.

作者信息

Pérez-Llarena Francisco José, Vázquez-Ucha Juan Carlos, Kerff Frédéric, Zamorano Laura, Miró Elisenda, Cabral María Póvoa, Fleites Ana, Lantero Marta, Martínez-Martínez Luis, Oliver Antonio, Galleni Moreno, Navarro Ferrán, Beceiro Alejandro, Bou Germán

机构信息

1 Servicio de Microbiología-INIBIC, Complejo Hospitalario Universitario A Coruña , A Coruña, Spain .

2 Centre d'Ingénierie des Protéines, Université de Liège , Liège, Belgium .

出版信息

Microb Drug Resist. 2018 Jun;24(5):527-533. doi: 10.1089/mdr.2017.0017. Epub 2017 Jun 30.

DOI:10.1089/mdr.2017.0017
PMID:28665771
Abstract

During a Spanish surveillance study, a natural variant of a CMY-type β-lactamase related to CMY-2 with a GluLeu insertion in the Ω-loop (designated CMY-54) was found to increase the minimum inhibitory concentractions to β-lactams in a clinical strain of Escherichia coli. The aim of this study was to characterize CMY-54 by genetic, microbiological, and biochemical analysis. The bla gene is encoded by a plasmid of around 100 kb that hybridizes with K and FIB probes. The genetic context of bla and bla genes was found to be very similar. E. coli expressing CMY-54 under isogenic conditions showed a clear fourfold to eightfold increase in MICs to penicillins, cefotaxime, ceftazidime, and aztreonam compared with CMY-2. The catalytic efficiencies of pure CMY-2 and CMY-54 proteins correlated with their microbiological parameters. CMY-2 protein was more resistant to thermal denaturation than CMY-54, indicating that the Ω-loop of CMY-54 may be wider and more relaxed and probably enables better accommodation of these antimicrobials. Otherwise, the higher stabilization of CMY-2 may induce a slight reduction of the dynamics of this enzyme and primarily affect the hydrolysis of some of the bulkiest antibiotics. In summary, the GluLeu insertion observed in CMY-54 compared to CMY-2 produces a β-lactamase with a distinctive catalytic efficacy for β-lactam antimicrobials likely caused by an increased flexibility slightly affecting the active site shape, highlighting the relevance of single mutations on the hydrolytic spectrum in class C β-lactamases.

摘要

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