N. T. Simon scite author profile

N. T. Simon

2Publications

44Citation Statements Received

94Citation Statements Given

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CEA Grenoble, The Ohio State University, Institut Pasteur

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

et al. 2018

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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.

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Utilization of exogenous siderophores and natural catechols by Listeria monocytogenes

Simon

Coulanges

André

et al. 1995

Appl Environ Microbiol

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N. T. Simon

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

Utilization of exogenous siderophores and natural catechols by Listeria monocytogenes

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