Background: MurE controls stereo chemical incorporation of Lysine or diaminopimelate into peptidoglycan stem peptides



Results: The structure of S.aureus MurE reveals an unexpected lack of specificity for Lysine within the active site.



Conclusion: Incorporation of Lysine is supported by the comparatively high concentration of cytoplasmic lysine, not enzyme specificity.



Significance: This study provides new perspectives in targeting Gram-positive peptidoglycan assembly for antimicrobial discovery

Barreteau

Basavannacharya

Battye

Bertrand

Boniface

Bouhss

Brünger

Bugg

Chen

Clancy

Clarke

Collaborative Computational Project, Number 4

Cressina

Crouvoisier

Cruickshank

De Lencastre

DeLano

Emsley

Ernst

Favini-Stabile

Figueiredo

Gardete

Girardin

Gordon

Gorrec

Huber

Hutton

Jones

Kabsch

Liebeke

Lloyd

Lundqvist

Lysenko

Matteï

McCoy

Mengin-Lecreulx

Mohammadi

Murshudov

Münch

Ornelas-Soares

Painter

Paradis-Bleau

Patin

Perdih

Read

Royet

Sauvage

Scheffers

Schneider

Schouten

Smith

Sosič

Sova

Thedieck

Vagin

Vollmer

Walker

Young

Zawadzke

English

PubMed

International audienceFormation of the peptidoglycan stem pentapeptide requires the insertion of both L and D amino acids by the ATP-dependent ligase enzymes MurC, -D, -E, and -F. The stereochemical control of the third position amino acid in the pentapeptide is crucial to maintain the fidelity of later biosynthetic steps contributing to cell morphology, antibiotic resistance, and pathogenesis. Here we determined the x-ray crystal structure of Staphylococcus aureus MurE UDP-N-acetylmuramoyl-L-alanyl-D-glutamate:meso-2,6-diaminopimelate ligase (MurE) (E.C. 6.3.2.7) at 1.8 Å resolution in the presence of ADP and the reaction product, UDP-MurNAc-L-Ala-γ-D-Glu-L-Lys. This structure provides for the first time a molecular understanding of how this Gram-positive enzyme discriminates between L-lysine and D,L-diaminopimelic acid, the predominant amino acid that replaces L-lysine in Gram-negative peptidoglycan. Despite the presence of a consensus sequence previously implicated in the selection of the third position residue in the stem pentapeptide in S. aureus MurE, the structure shows that only part of this sequence is involved in the selection of L-lysine. Instead, other parts of the protein contribute substrate-selecting residues, resulting in a lysine-binding pocket based on charge characteristics. Despite the absolute specificity for L-lysine, S. aureus MurE binds this substrate relatively poorly. In vivo analysis and metabolomic data reveal that this is compensated for by high cytoplasmic L-lysine concentrations. Therefore, both metabolic and structural constraints maintain the structural integrity of the staphylococcal peptidoglycan. This study provides a novel focus for S. aureus-directed antimicrobials based on dual targeting of essential amino acid biogenesis and its linkage to cell wall assembly

Ruane, Karen M

Lloyd, Adrian J

Fülöp, Vilmos

Barreteau, Hélène

Boniface, Audrey

Dementin, Sébastien

Blanot, Didier

Mengin-Lecreulx, Dominique

Gobec, Stanislav

Dessen, Andréa

Roper, David I

Hal - Université Grenoble Alpes

Specificity determinants for lysine incorporation in Staphylococcus aureus peptidoglycan as revealed by the structure of a MurE enzyme ternary complex.

Ruane, Karen M.

Lloyd, Adrian J.

Dowson, Christopher G.

Roper, David I.

Warwick Research Archives Portal Repository

Peptidoglycan structure and architecture.

Topological analysis of the MraY protein catalysing the first membrane step of peptidoglycan synthesis.

Specificity determinants for lysine incorporation in staphylococcus aureus peptidoglycan as revealed by the structure of a MurE enzyme ternary complex

HAL-CEA

HAL: Hyper Article en Ligne

Karen M. Ruane

Adrian J. Lloyd

Vilmos Fülöp

Christopher G. Dowson

Hélène Barreteau

Audrey Boniface

Sébastien Dementin

Didier Blanot

Dominique Mengin-Lecreulx

Stanislav Gobec

Andréa Dessen

David I. Roper

Crossref

Journal of Biological Chemistry

Specificity Determinants for Lysine Incorporation in Staphylococcus aureus Peptidoglycan as Revealed by the Structure of a MurE Enzyme Ternary Complex

http://wrap.warwick.ac.uk/57922/1/WRAP_Fulop_J.%20Biol.%20Chem.-2013-Ruane-33439-48.pdf

Specificity determinants for lysine incorporation in staphylococcus aureus peptidoglycan as revealed by the structure of a MurE enzyme ternary complex

Abstract

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Hal - Université Grenoble Alpes

Warwick Research Archives Portal Repository

HAL-CEA

HAL: Hyper Article en Ligne

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