A Peptidoglycan Fragment Triggers β-lactam Resistance in Bacillus licheniformis

Amoroso, Ana Maria; Boudet, Julien; Berzigotti, Stéphanie; Duval, Valérie; Teller, Nathalie; Mengin‐Lecreulx, Dominique; Luxen, André; Simorre, Jean-Pierre; Joris, Bernard

doi:10.1371/journal.ppat.1002571

Cited by 47 publications

(40 citation statements)

References 61 publications

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“…In addition, peptidoglycan fragments are found to be involved in the regulation of ␤-lactamase expression in Gram-positive bacteria, although the regulatory mechanism is quite different from that of AmpC (17). These observations suggest that the involvement of peptidoglycan recycling is a generic mechanism in ␤-lactamase expression.…”

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confidence: 95%

Distinct Roles of Major Peptidoglycan Recycling Enzymes in β-Lactamase Production in Shewanella oneidensis

Yin

Mao

et al. 2014

Antimicrob Agents Chemother

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c ␤-Lactam antibiotics were the earliest discovered and are the most widely used group of antibiotics that work by inactivating penicillin-binding proteins to inhibit peptidoglycan biosynthesis. As one of the most efficient defense strategies, many bacteria produce ␤-lactam-degrading enzymes, ␤-lactamases, whose biochemical functions and regulation have been extensively studied. A signal transduction pathway for ␤-lactamase induction by ␤-lactam antibiotics, consisting of the major peptidoglycan recycling enzymes and the LysR-type transcriptional regulator, AmpR, has been recently unveiled in some bacteria. Because inactivation of some of these proteins, especially the permease AmpG and the ␤-hexosaminidase NagZ, results in substantially elevated susceptibility to the antibiotics, these have been recognized as potential therapeutic targets. Here, we show a contrasting scenario in Shewanella oneidensis, in which the homologue of AmpR is absent. Loss of AmpG or NagZ enhances ␤-lactam resistance drastically, whereas other identified major peptidoglycan recycling enzymes are dispensable. Moreover, our data indicate that there exists a parallel signal transduction pathway for ␤-lactamase induction, which is independent of either AmpG or NagZ.

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confidence: 95%

Distinct Roles of Major Peptidoglycan Recycling Enzymes in β-Lactamase Production in Shewanella oneidensis

Yin

Mao

et al. 2014

Antimicrob Agents Chemother

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“…This cleavage would render the dimeric repressor inactive and release it from its DNA-binding site. A similar effect of inhibitor inactivation, which was not based, however, on a proteolytic pathway but on the intracellular presence of a short dipeptidic peptidoglycan fragment induced by BLA stress, has been recently described for B. licheniformis (28). Finally, release of transcriptional repression would elicit biosynthesis of MecA/BlaZ.…”

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confidence: 55%

Structure-Function Studies of the Staphylococcal Methicillin Resistance Antirepressor MecR2

Arede

Botelho

Guevara

et al. 2013

Journal of Biological Chemistry

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Background: PBP2a-based methicillin resistance in S. aureus is regulated by the protein MecR2. Results: The structure of MecR2 shows a dimeric multidomain ROK family protein, which nonspecifically binds oligonucleotides but not sugar ligands. Conclusion: MecR2 represents an evolution within ROK proteins to give rise to a protein-binding antirepressor. Significance: The present results pave the way for the design of new antimicrobials.

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“…This cleavage event is believed to be initiated by the b-lactam acylation of BlaRs, resulting in conformational changes in the transmembrane bundle that carry the signal across the bilayer (Zhang et al 2001). Although the ultimate result of BlaRp activation is the cleavage of BlaI, it is not yet certain whether BlaI is the direct substrate of BlaRp or the end result of a proteolytic relay (Llarrull and Mobashery 2012;Amoroso et al 2012).…”

Section: Sensor-/transducer-mediated Regulation Of B-lactam Resistancementioning

confidence: 99%

“…These peptides and their breakdown products are postulated to be transported to the cytoplasm via conserved ABC transporters or the phosphotransferase system for recycling (Reith and Mayer 2011). Recently, it has been demonstrated that in B. Licheniformis, a cell-wall-derived dipeptide fragment, g-D-Glu-m-DAP, is capable of binding the BlaI (MecI) repressor, leading to its dissociation from the bla operon and subsequent induction of the b-lactamase, BlaP (Amoroso et al 2012). Although the exact pathway for the generation of the dipeptide has not yet been discerned, this finding draws an interesting parallel between recycling and antibiotic resistance in Gram-positive and Gram-negative bacteria.…”

Section: Pg Recycling and Regulation Of B-lactam Resistancementioning

confidence: 99%

The Mechanisms of Resistance to β-Lactam Antibiotics

King

Sobhanifar

Strynadka

2014

Handbook of Antimicrobial Resistance

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Bacterial diseases have had an enormous impact on human health and continue to be a major focus in modern medicine. The most widespread class of human antibacterials is the b-lactams that target the transpeptidase enzymes, which are responsible for cross-linking the peptidoglycan cell wall. There are over 34 FDA-approved b-lactams which together constitute $50 % of all antibiotic prescriptions worldwide (Tahlan K and Jensen SE, J Antibiot (Tokyo) 66:401-410, 2013). However, bacteria have gained resistance mechanisms to overcome all major classes of b-lactam antibiotics to date. In this chapter, we will address the major mechanisms of bacterial resistance to the b-lactams and highlight some of the recent advances in circumventing this resistance.

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A Peptidoglycan Fragment Triggers β-lactam Resistance in Bacillus licheniformis

Cited by 47 publications

References 61 publications

Distinct Roles of Major Peptidoglycan Recycling Enzymes in β-Lactamase Production in Shewanella oneidensis

Distinct Roles of Major Peptidoglycan Recycling Enzymes in β-Lactamase Production in Shewanella oneidensis

Structure-Function Studies of the Staphylococcal Methicillin Resistance Antirepressor MecR2

The Mechanisms of Resistance to β-Lactam Antibiotics

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