Structure of the essential peptidoglycan amidotransferase MurT/GatD complex from Streptococcus pneumoniae

Publication date

2018-12-01

Authors

Morlot, Cécile
Straume, Daniel
Peters, Katharina
Hegnar, Olav A.
Simon, Nolwenn
Villard, Anne-Marie
Contreras-Martel, Carlos
Leisico, Francisco
Breukink, EefjanISNI 0000000392861563
Gravier-Pelletier, Christine

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Abstract

The universality of peptidoglycan in bacteria underlies the broad spectrum of many successful antibiotics. However, in our times of widespread resistance, the diversity of peptidoglycan modifications offers a variety of new antibacterials targets. In some Gram-positive species such as Streptococcus pneumoniae, Staphylococcus aureus, or Mycobacterium tuberculosis, the second residue of the peptidoglycan precursor, D-glutamate, is amidated into iso-D-glutamine by the essential amidotransferase MurT/GatD complex. Here, we present the structure of this complex at 3.0 Å resolution. MurT has central and C-terminal domains similar to Mur ligases with a cysteine-rich insertion, which probably binds zinc, contributing to the interface with GatD. The mechanism of amidation by MurT is likely similar to the condensation catalyzed by Mur ligases. GatD is a glutaminase providing ammonia that is likely channeled to the MurT active site through a cavity network. The structure and assay presented here constitute a knowledge base for future drug development studies.

Keywords

ammonia, GatD glutaminase, glutaminase, glutamine, ligase, MurT ligase, peptidoglycan, unclassified drug, zinc, amidation, article, carboxy terminal sequence, enzyme active site, enzyme activity, enzyme kinetics, nonhuman, operon, pH, Streptococcus pneumoniae, SDG 3 - Good Health and Well-being

Citation

Morlot, C, Straume, D, Peters, K, Hegnar, O A, Simon, N, Villard, A-M, Contreras-Martel, C, Leisico, F, Breukink, E, Gravier-Pelletier, C, Le Corre, L, Vollmer, W, Pietrancosta, N, Håvarstein, L S & Zapun, A 2018, 'Structure of the essential peptidoglycan amidotransferase MurT/GatD complex from Streptococcus pneumoniae', Nature Communications, vol. 9, no. 1, 3180. https://doi.org/10.1038/s41467-018-05602-w