Recognition of Peptidoglycan Fragments by the Transpeptidase PBP4 From Staphylococcus aureus

Peptidoglycan (PG) is an essential component of the cell envelope, maintaining bacterial cell shape and protecting it from bursting due to turgor pressure. The monoderm bacterium Staphylococcus aureus has a highly cross-linked PG, with ~90% of peptide stems participating in DD-cross-links and up to...

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Autores principales: Maya-Martinez, Roberto, Alexander, J. Andrew N., Otten, Christian F., Ayala, Isabel, Vollmer, Daniela, Gray, Joe, Bougault, Catherine M., Burt, Alister, Laguri, Cédric, Fonvielle, Matthieu, Arthur, Michel, Strynadka, Natalie C. J., Vollmer, Waldemar, Simorre, Jean-Pierre
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2019
Materias:
Microbiology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6346638/
https://www.ncbi.nlm.nih.gov/pubmed/30713527
http://dx.doi.org/10.3389/fmicb.2018.03223
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author Maya-Martinez, Roberto
Alexander, J. Andrew N.
Otten, Christian F.
Ayala, Isabel
Vollmer, Daniela
Gray, Joe
Bougault, Catherine M.
Burt, Alister
Laguri, Cédric
Fonvielle, Matthieu
Arthur, Michel
Strynadka, Natalie C. J.
Vollmer, Waldemar
Simorre, Jean-Pierre
author_facet Maya-Martinez, Roberto
Alexander, J. Andrew N.
Otten, Christian F.
Ayala, Isabel
Vollmer, Daniela
Gray, Joe
Bougault, Catherine M.
Burt, Alister
Laguri, Cédric
Fonvielle, Matthieu
Arthur, Michel
Strynadka, Natalie C. J.
Vollmer, Waldemar
Simorre, Jean-Pierre
author_sort Maya-Martinez, Roberto
collection PubMed
description Peptidoglycan (PG) is an essential component of the cell envelope, maintaining bacterial cell shape and protecting it from bursting due to turgor pressure. The monoderm bacterium Staphylococcus aureus has a highly cross-linked PG, with ~90% of peptide stems participating in DD-cross-links and up to 15 peptide stems connected with each other. These cross-links are formed in transpeptidation reactions catalyzed by penicillin-binding proteins (PBPs) of classes A and B. Most S. aureus strains have three housekeeping PBPs with this function (PBP1, PBP2, and PBP3) but MRSA strains have acquired a third class B PBP, PBP2a, which is encoded by the mecA gene and required for the expression of high-level resistance to β-lactams. Another housekeeping PBP of S. aureus is PBP4, which belongs to the class C PBPs, and hence would be expected to have PG hydrolase (DD-carboxypeptidase or DD-endopeptidase) activity. However, previous works showed that, unexpectedly, PBP4 has transpeptidase activity that significantly contributes to both the high level of cross-linking in the PG of S. aureus and to the low level of β-lactam resistance in the absence of PBP2a. To gain insights into this unusual activity of PBP4, we studied by NMR spectroscopy its interaction in vitro with different substrates, including intact peptidoglycan, synthetic peptide stems, muropeptides, and long glycan chains with uncross-linked peptide stems. PBP4 showed no affinity for the complex, intact peptidoglycan or the smallest isolated peptide stems. Transpeptidase activity of PBP4 was verified with the disaccharide peptide subunits (muropeptides) in vitro, producing cyclic dimer and multimer products; these assays also showed a designed PBP4(S75C) nucleophile mutant to be inactive. Using this inactive but structurally highly similar variant, liquid-state NMR identified two interaction surfaces in close proximity to the central nucleophile position that can accommodate the potential donor and acceptor stems for the transpeptidation reaction. A PBP4:muropeptide model structure was built from these experimental restraints, which provides new mechanistic insights into mecA independent resistance to β-lactams in S. aureus.
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spelling pubmed-63466382019-02-01 Recognition of Peptidoglycan Fragments by the Transpeptidase PBP4 From Staphylococcus aureus Maya-Martinez, Roberto Alexander, J. Andrew N. Otten, Christian F. Ayala, Isabel Vollmer, Daniela Gray, Joe Bougault, Catherine M. Burt, Alister Laguri, Cédric Fonvielle, Matthieu Arthur, Michel Strynadka, Natalie C. J. Vollmer, Waldemar Simorre, Jean-Pierre Front Microbiol Microbiology Peptidoglycan (PG) is an essential component of the cell envelope, maintaining bacterial cell shape and protecting it from bursting due to turgor pressure. The monoderm bacterium Staphylococcus aureus has a highly cross-linked PG, with ~90% of peptide stems participating in DD-cross-links and up to 15 peptide stems connected with each other. These cross-links are formed in transpeptidation reactions catalyzed by penicillin-binding proteins (PBPs) of classes A and B. Most S. aureus strains have three housekeeping PBPs with this function (PBP1, PBP2, and PBP3) but MRSA strains have acquired a third class B PBP, PBP2a, which is encoded by the mecA gene and required for the expression of high-level resistance to β-lactams. Another housekeeping PBP of S. aureus is PBP4, which belongs to the class C PBPs, and hence would be expected to have PG hydrolase (DD-carboxypeptidase or DD-endopeptidase) activity. However, previous works showed that, unexpectedly, PBP4 has transpeptidase activity that significantly contributes to both the high level of cross-linking in the PG of S. aureus and to the low level of β-lactam resistance in the absence of PBP2a. To gain insights into this unusual activity of PBP4, we studied by NMR spectroscopy its interaction in vitro with different substrates, including intact peptidoglycan, synthetic peptide stems, muropeptides, and long glycan chains with uncross-linked peptide stems. PBP4 showed no affinity for the complex, intact peptidoglycan or the smallest isolated peptide stems. Transpeptidase activity of PBP4 was verified with the disaccharide peptide subunits (muropeptides) in vitro, producing cyclic dimer and multimer products; these assays also showed a designed PBP4(S75C) nucleophile mutant to be inactive. Using this inactive but structurally highly similar variant, liquid-state NMR identified two interaction surfaces in close proximity to the central nucleophile position that can accommodate the potential donor and acceptor stems for the transpeptidation reaction. A PBP4:muropeptide model structure was built from these experimental restraints, which provides new mechanistic insights into mecA independent resistance to β-lactams in S. aureus. Frontiers Media S.A. 2019-01-18 /pmc/articles/PMC6346638/ /pubmed/30713527 http://dx.doi.org/10.3389/fmicb.2018.03223 Text en Copyright © 2019 Maya-Martinez, Alexander, Otten, Ayala, Vollmer, Gray, Bougault, Burt, Laguri, Fonvielle, Arthur, Strynadka, Vollmer and Simorre. http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Microbiology
Maya-Martinez, Roberto
Alexander, J. Andrew N.
Otten, Christian F.
Ayala, Isabel
Vollmer, Daniela
Gray, Joe
Bougault, Catherine M.
Burt, Alister
Laguri, Cédric
Fonvielle, Matthieu
Arthur, Michel
Strynadka, Natalie C. J.
Vollmer, Waldemar
Simorre, Jean-Pierre
Recognition of Peptidoglycan Fragments by the Transpeptidase PBP4 From Staphylococcus aureus
title Recognition of Peptidoglycan Fragments by the Transpeptidase PBP4 From Staphylococcus aureus
title_full Recognition of Peptidoglycan Fragments by the Transpeptidase PBP4 From Staphylococcus aureus
title_fullStr Recognition of Peptidoglycan Fragments by the Transpeptidase PBP4 From Staphylococcus aureus
title_full_unstemmed Recognition of Peptidoglycan Fragments by the Transpeptidase PBP4 From Staphylococcus aureus
title_short Recognition of Peptidoglycan Fragments by the Transpeptidase PBP4 From Staphylococcus aureus
title_sort recognition of peptidoglycan fragments by the transpeptidase pbp4 from staphylococcus aureus
topic Microbiology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6346638/
https://www.ncbi.nlm.nih.gov/pubmed/30713527
http://dx.doi.org/10.3389/fmicb.2018.03223
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