AI Article Synopsis
- The synthesis of bacterial peptidoglycan involves four key enzymes known as Mur ligases, with MurD playing a critical role by adding d-glutamic acid to UDP-MurNAc-l-Ala using ATP.
- The 3D structure of E. coli MurD has been extensively studied, providing insights into its substrate specificity, reaction mechanisms, and interactions with inhibitors.
- The review also explores MurD orthologs in other species and discusses potential new antibacterial agents developed from various classes of MurD inhibitors.
Article Abstract
The synthesis of the peptide stem of bacterial peptidoglycan involves four enzymes, the Mur ligases (MurC, D, E and F). Among them, MurD is responsible for the ATP-dependent addition of d-glutamic acid to UDP-MurNAc-l-Ala, a reaction which involves acyl-phosphate and tetrahedral intermediates. Like most enzymes of peptidoglycan biosynthesis, MurD constitutes an attractive target for the design and synthesis of new antibacterial agents. Escherichia coli MurD has been the first Mur ligase for which the tridimensional (3D) structure was solved. Thereafter, several co-crystal structures with different ligands or inhibitors were released. In the present review, we will deal with work performed on substrate specificity, reaction mechanism and 3D structure of E. coli MurD. Then, a part of the review will be devoted to recent work on MurD orthologs from species other than E. coli and to cellular organization of Mur ligases and in vivo regulation of the MurD activity. Finally, we will review the different classes of MurD inhibitors that have been designed and assayed to date with the hope of obtaining new antibacterial compounds.
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| http://dx.doi.org/10.1515/bmc-2013-0024 | DOI Listing |
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