A New Mechanism for β‐Lactamases: Class D Enzymes Degrade 1β‐Methyl Carbapenems through Lactone Formation |
| |
| Authors: | Dr Christopher T Lohans Emma van?Groesen Kiran Kumar Catherine L Tooke Dr James Spencer Prof?Dr Robert S Paton Dr Jürgen Brem Prof?Dr Christopher J Schofield |
| |
| Institution: | 1. Department of Chemistry, University of Oxford, Oxford, UK;2. School of Cellular and Molecular Medicine, University of Bristol, Bristol, UK |
| |
| Abstract: | β‐Lactamases threaten the clinical use of carbapenems, which are considered antibiotics of last resort. The classical mechanism of serine carbapenemase catalysis proceeds through hydrolysis of an acyl‐enzyme intermediate. We show that class D β‐lactamases also degrade clinically used 1β‐methyl‐substituted carbapenems through the unprecedented formation of a carbapenem‐derived β‐lactone. β‐Lactone formation results from nucleophilic attack of the carbapenem hydroxyethyl side chain on the ester carbonyl of the acyl‐enzyme intermediate. The carbapenem‐derived lactone products inhibit both serine β‐lactamases (particularly class D) and metallo‐β‐lactamases. These results define a new mechanism for the class D carbapenemases, in which a hydrolytic water molecule is not required. |
| |
| Keywords: | antibiotics β -lactamases carbapenems hydrolases lactones |
|
|
