Deletion of
            <i>liaR</i>
            Reverses Daptomycin Resistance in Enterococcus faecium Independent of the Genetic Background

Panesso, Diana; Reyes, Jinnethe; Gaston, Elizabeth P.; Deal, M.; Londoño, Alejandra; Nigo, Masayuki; Munita, José M.; Miller, William R.; Shamoo, Yousif; Tran, Truc T.; Arias, César A.

doi:10.1128/aac.01073-15

Cited by 42 publications

(42 citation statements)

References 39 publications

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“…To determine whether c-di-AMP signaling is present in other enterococcal strains, daptomycin-tolerant and vancomycin-resistant Enterococcus faecium clinical isolate HOU503 and its fusidic acid-resistant derivative E. faecium HOU503F were tested (Table 1) (27). The c-di-AMP levels of E. faecium HOU503 and E. faecium HOU503F were 766 Ϯ 318 and 542 Ϯ 133 pM/OD 600 at late exponential phase (OD 600 , ϳ1.2) ( Table 1 and Fig.…”

Section: Resultsmentioning

confidence: 99%

“…To demonstrate that changes in LiaFSR signaling lead to changes in c-di-AMP more broadly, we measured the c-di-AMP levels in nonpolar liaR deletion mutants of E. faecium strains HOU503F and R497F (E. faecium HOU503F_ΔliaR and R497F_ΔliaR, Table 1) which are tolerant of and resistant to daptomycin (27). As observed with E. faecalis, deletion of liaR in E. faecium HOU503F_ΔliaR and R497F_ΔliaR showed modest increases in c-di-AMP levels compared to E. faecium HOU503F and R497F (622 Ϯ 104 pM/OD 600 versus 542 Ϯ 133 pM/OD 600 and 736 Ϯ 186 pM/OD 600 versus 549 Ϯ 150 pM/OD 600 , Fig.…”

Section: C-di-amp Signaling In Enterococcimentioning

confidence: 99%

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A Novel Phosphodiesterase of the GdpP Family Modulates Cyclic di-AMP Levels in Response to Cell Membrane Stress in Daptomycin-Resistant Enterococci

Wang

Davlieva

Reyes

et al. 2017

Antimicrob Agents Chemother

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Substitutions in the LiaFSR membrane stress pathway are frequently associated with the emergence of antimicrobial peptide resistance in both Enterococcus faecalis and Enterococcus faecium. Cyclic di-AMP (c-di-AMP) is an important signal molecule that affects many aspects of bacterial physiology, including stress responses. We have previously identified a mutation in a gene (designated yybT) in E. faecalis that was associated with the development of daptomycin resistance, resulting in a change at position 440 (yybT I440S ) in the predicted protein. Here, we show that intracellular c-di-AMP signaling is present in enterococci, and on the basis of in vitro physicochemical characterization, we show that E. faecalis yybT encodes a cyclic dinucleotide phosphodiesterase of the GdpP family that exhibits specific activity toward c-di-AMP by hydrolyzing it to 5=pApA. The E. faecalis GdpP I440S substitution reduces c-di-AMP phosphodiesterase activity more than 11-fold, leading to further increases in c-di-AMP levels. Additionally, deletions of liaR (encoding the response regulator of the LiaFSR system) that lead to daptomycin hypersusceptibility in both E. faecalis and E. faecium also resulted in increased c-di-AMP levels, suggesting that changes in the LiaFSR stress response pathway are linked to broader physiological changes. Taken together, our data show that modulation of c-di-AMP pools is strongly associated with antibiotic-induced cell membrane stress responses via changes in GdpP activity or signaling through the LiaFSR system.

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Section: Resultsmentioning

confidence: 99%

Section: C-di-amp Signaling In Enterococcimentioning

confidence: 99%

A Novel Phosphodiesterase of the GdpP Family Modulates Cyclic di-AMP Levels in Response to Cell Membrane Stress in Daptomycin-Resistant Enterococci

Wang

Davlieva

Reyes

et al. 2017

Antimicrob Agents Chemother

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“…It is also significant that genes protective against daptomycin (liaXYZ) are highly upregulated in response to chlorhexidine. It was recently demonstrated that deletion of liaR, encoding an activator of liaXYZ expression (45), restores daptomycin susceptibility to daptomycin-nonsusceptible enterococci (76). Further studies will be required to determine whether gene expression "priming" by chlorhexidine impacts treatment outcomes with daptomycin, or if frequent exposure to subinhibitory chlorhexidine is selective for strains that constitutively activate liaXYZ.…”

Section: Discussionmentioning

confidence: 99%

Chlorhexidine Induces VanA-Type Vancomycin Resistance Genes in Enterococci

Bhardwaj

Ziegler

Palmer

2016

Antimicrob Agents Chemother

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Chlorhexidine is a bisbiguanide antiseptic used for infection control. Vancomycin-resistant E. faecium (VREfm) is among the leading causes of hospital-acquired infections. VREfm may be exposed to chlorhexidine at supra-and subinhibitory concentrations as a result of chlorhexidine bathing and chlorhexidine-impregnated central venous catheter use. We used RNA sequencing to investigate how VREfm responds to chlorhexidine gluconate exposure. Among the 35 genes upregulated >10-fold after 15 min of exposure to the MIC of chlorhexidine gluconate were those encoding VanA-type vancomycin resistance (vanHAX) and those associated with reduced daptomycin susceptibility (liaXYZ). We confirmed that vanA upregulation was not strain or species specific by querying other VanA-type VRE. VanB-type genes were not induced. The vanH promoter was found to be responsive to subinhibitory chlorhexidine gluconate in VREfm, as was production of the VanX protein. Using vanH reporter experiments with Bacillus subtilis and deletion analysis in VREfm, we found that this phenomenon is VanR dependent. Deletion of vanR did not result in increased chlorhexidine susceptibility, demonstrating that vanHAX induction is not protective against chlorhexidine. As expected, VanA-type VRE is more susceptible to ceftriaxone in the presence of sub-MIC chlorhexidine. Unexpectedly, VREfm is also more susceptible to vancomycin in the presence of subinhibitory chlorhexidine, suggesting that chlorhexidine-induced gene expression changes lead to additional alterations in cell wall synthesis. We conclude that chlorhexidine induces expression of VanA-type vancomycin resistance genes and genes associated with daptomycin nonsusceptibility. Overall, our results indicate that the impacts of subinhibitory chlorhexidine exposure on hospital-associated pathogens should be further investigated in laboratory studies.

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“…116 In such strains, the activation of LiaRS greatly reduces the efficiency of daptomycin to bacterial cells. 117 When activated, LiaRS induces the expression of LiaI and LiaH, which colocalize within segregated domains in the cytoplasmic membrane. 118 The phenotypic effects of these effector molecules, and accordingly their role in daptomycin resistance, are not yet understood.…”

Section: Activation Of Liarsmentioning

confidence: 99%

The action mechanism of daptomycin

Taylor

Palmer

2016

Bioorganic & Medicinal Chemistry

210

172

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Daptomycin is a lipopeptide antibiotic produced by the soil bacterium Streptomyces roseosporus that is clinically used to treat severe infections with Grampositive bacteria. In this review, we discuss the mode of action of this important antibiotic. Although daptomycin is structurally related to amphomycin and similar lipopeptides that inhibit peptidoglycan biosynthesis, experimental studies have not produced clear evidence that daptomycin shares their action mechanism. Instead, the best characterized effect of daptomycin is the permeabilization and depolarization of the bacterial cell membrane. This activity, which can account for daptomycin's bactericidal effect, correlates with the level of phosphatidylglycerol (PG) in the membrane. Accordingly, reduced synthesis of PG or its increased conversion to lysyl-PG promotes bacterial resistance to daptomycin. While other resistance mechanisms suggest that daptomycin may indeed directly interfere with cell wall synthesis or cell division, such effects still await direct experimental confirmation. Daptomycin's complex structure and biosynthesis have hampered the analysis of its structure activity relationships. Novel methods of total synthesis, including a recent one that is carried out entirely on a solid phase, will enable a more thorough and systematic exploration of the sequence space.

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Deletion of liaR Reverses Daptomycin Resistance in Enterococcus faecium Independent of the Genetic Background

Cited by 42 publications

References 39 publications

A Novel Phosphodiesterase of the GdpP Family Modulates Cyclic di-AMP Levels in Response to Cell Membrane Stress in Daptomycin-Resistant Enterococci

A Novel Phosphodiesterase of the GdpP Family Modulates Cyclic di-AMP Levels in Response to Cell Membrane Stress in Daptomycin-Resistant Enterococci

Chlorhexidine Induces VanA-Type Vancomycin Resistance Genes in Enterococci

The action mechanism of daptomycin

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