Toxin–antitoxin systems are ubiquitous and plasmid-encoded in vancomycin-resistant enterococci

Moritz, Elizabeth M.; Hergenrother, Paul J.

doi:10.1073/pnas.0601168104

Cited by 124 publications

(132 citation statements)

References 70 publications

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“…TA-driven RNA interference has been implicated in the regulation of virulence and antibiotic resistance in numerous pathogens including M. tuberculosis 16 , S. aureus 15,20 , Yersinia pestis 21 , Helicobacter pylori 22 , Streptococcus mutans 23 and C. difficile 17 , and also among enterococci 24 . However, the occurrence of this mechanism remains largely speculative, and the very attractive concept of global regulation of virulence factor expression by TA systems in pathogenic bacteria still awaits thorough experimental characterization.…”

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confidence: 99%

A regulatory role for Staphylococcus aureus toxin–antitoxin system PemIKSa

et al. 2013

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Toxin-antitoxin systems were shown to be involved in plasmid maintenance when they were initially discovered, but other roles have been demonstrated since. Here we identify and characterize a novel toxin-antitoxin system (pemIK Sa ) located on Staphylococcus aureus plasmid pCH91. The toxin (PemK Sa ) is a sequence-specific endoribonuclease recognizing the tetrad sequence UkAUU, and the antitoxin (PemI Sa ) inhibits toxin activity by physical interaction. Although the toxin-antitoxin system is responsible for stable plasmid maintenance our data suggest the participation of pemIK Sa in global regulation of staphylococcal virulence by alteration of the translation of large pools of genes. We propose a common mechanism of reversible activation of toxin-antitoxin systems based on antitoxin transcript resistance to toxin cleavage. Elucidation of this mechanism is particularly interesting because reversible activation is a prerequisite for the proposed general regulatory role of toxin-antitoxin systems.

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confidence: 99%

A regulatory role for Staphylococcus aureus toxin–antitoxin system PemIKSa

et al. 2013

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“…The contribution of plasmids to antibiotic resistance in bacterial pathogens has led to the proposal that agents inhibiting the replication of these extrachromosomal DNAs, or activating their PSK systems, could be exploited to kill these organisms directly and selectively (11)(12)(13). Our work raises concerns against this approach in the case of R1 and its kis-kid TA pair.…”

Section: Kid Inhibits Cell Division In E Coli and Does Not Halt Protmentioning

confidence: 70%

“…The link of these systems to PSK and the exiguous list of alternatives in the pipeline have led some to propose that chemicals activating these TA pairs may constitute a powerful antibiotic approach against these organisms (5,(11)(12)(13). However, the appropriateness of these TA pairs as therapeutic targets requires unequivocal understanding of their function in plasmids.…”

mentioning

confidence: 99%

Toxin Kid uncouples DNA replication and cell division to enforce retention of plasmid R1 in Escherichia coli cells

Pimentel

Nair

Bermejo-Rodríguez

et al. 2014

Proc. Natl. Acad. Sci. U.S.A.

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Worldwide dissemination of antibiotic resistance in bacteria is facilitated by plasmids that encode postsegregational killing (PSK) systems. These produce a stable toxin (T) and a labile antitoxin (A) conditioning cell survival to plasmid maintenance, because only this ensures neutralization of toxicity. Shortage of antibiotic alternatives and the link of TA pairs to PSK have stimulated the opinion that premature toxin activation could be used to kill these recalcitrant organisms in the clinic. However, validation of TA pairs as therapeutic targets requires unambiguous understanding of their mode of action, consequences for cell viability, and function in plasmids. Conflicting with widespread notions concerning these issues, we had proposed that the TA pair kis-kid (killing suppressor-killing determinant) might function as a plasmid rescue system and not as a PSK system, but this remained to be validated. Here, we aimed to clarify unsettled mechanistic aspects of Kid activation, and of the effects of this for kis-kid-bearing plasmids and their host cells. We confirm that activation of Kid occurs in cells that are about to lose the toxin-encoding plasmid, and we show that this provokes highly selective restriction of protein outputs that inhibits cell division temporarily, avoiding plasmid loss, and stimulates DNA replication, promoting plasmid rescue. Kis and Kid are conserved in plasmids encoding multiple antibiotic resistance genes, including extended spectrum β-lactamases, for which therapeutic options are scarce, and our findings advise against the activation of this TA pair to fight pathogens carrying these extrachromosomal DNAs.PemK | mRNA interferase | parD | plasmid stability | RNase

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“…Most proteic TA systems are characterized by two small (8)(9)(10)(11)(12)(13)(14)(15) proteins, a stable toxin and a labile antitoxin, and genes encoding these proteins have been identified on a wide range of bacterial chromosomes and plasmids [4,5]. If both proteins are actively being produced by the bacterial cell, the antitoxin binds the toxin and inhibits its toxic activity.…”

Section: Introductionmentioning

confidence: 99%

“…Given that a large percentage of genes that mediate resistance to antibiotics are found on extrachromosomal DNA such as plasmids [14,15], coupled with the ability of TA systems to stabilize plasmids, it has been speculated that pharmacological disruption of the toxin-antitoxin protein-protein interaction could unleash the toxin and be a novel antibacterial strategy [2,5,16,17]. It was not until recently, however, that it was discovered that TA systems are indeed ubiquitous on plasmids that reside in a common bacterial pathogen that is refractory to most antibiotics, vancomycin-resistant enterococci (VRE) [5].…”

Section: Introductionmentioning

confidence: 99%

A continuous fluorometric assay for the assessment of MazF ribonuclease activity

Wang

Hergenrother

2007

Analytical Biochemistry

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Plasmids maintain themselves in their bacterial host through several different mechanisms, one of which involves the synthesis of plasmid-encoded toxin and antitoxin proteins. When the plasmid is present the antitoxin binds to and neutralizes the toxin. If a plasmid-free daughter cell arises, however, the labile antitoxin is degraded (and not replenished) and the toxin kills the cell from within. These toxin-antitoxin (TA) systems thereby function as post-segregational killing systems, and the disruption of the TA interaction represents an intriguing antibacterial strategy. It was recently discovered that the genes for one particular TA system, MazEF, are ubiquitous on plasmids isolated from clinical vancomycin-resistant enterococci (VRE) strains. It thus appears that small molecule disruptors of the MazEF interaction have potential as antibacterial agents. The MazF toxin protein is known to be a ribonuclease. Unfortunately, traditional methods for the assessment of MazF activity rely on the use of radiolabeled substrates followed by analysis with polyacrylamide gel electrophoresis. Described herein is a simple and convenient continuous assay for the assessment of MazF activity. This assay utilizes an oligonucleotide with a fluorophore on the 5′-end and a quencher on the 3′-end, and processing of this substrate by MazF results in a large increase in the fluorescence signal. Through this assay we have for the first time determined a K M and V max for this enzyme, and have also found that MazF is not inhibited by standard ribonuclease inhibitors. This assay will be useful to those interested in the biochemistry of the MazF family of toxins and the disruption of MazE-MazF.

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Toxin–antitoxin systems are ubiquitous and plasmid-encoded in vancomycin-resistant enterococci

Cited by 124 publications

References 70 publications

A regulatory role for Staphylococcus aureus toxin–antitoxin system PemIKSa

A regulatory role for Staphylococcus aureus toxin–antitoxin system PemIKSa

Toxin Kid uncouples DNA replication and cell division to enforce retention of plasmid R1 in Escherichia coli cells

A continuous fluorometric assay for the assessment of MazF ribonuclease activity

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