The Two-Component System ChtRS Contributes to Chlorhexidine Tolerance in Enterococcus faecium

Prieto, Ana M. Guzmán; Wijngaarden, Jessica; Braat, Johanna C.; Rogers, Malbert R. C.; Majoor, Eline; Brouwer, Eric; Zhang, Xinglin; Bayjanov, Jumamurat R.; Bonten, Marc J. M.; Willems, Rob J. L.; Schaik, Willem van

doi:10.1128/aac.02122-16

Cited by 33 publications

(18 citation statements)

References 60 publications

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“…Earlier studies with other oral streptococci, including Streptococcus sanguinis and Streptococcus mitis, showed that repeated exposure to CHX resulted in increased MICs to CHX, but these findings were not deemed to be of clinical significance (13)(14)(15)(16)(17). In enterococci, increased tolerance to antiseptics such as CHX in hospital settings has inspired research into the mechanisms for increased CHX tolerance, including studies of CHX effects on the transcriptome (18) and analysis of the impact of CHX on a transposon mutant library (19). More specifically, Bhardwaj and colleagues (18) used transcriptome sequencing (RNA-Seq) to show that VanA-type vancomycin resistance genes are upregulated in Enterococcus faecium following exposure to CHX.…”

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confidence: 99%

“…More specifically, Bhardwaj and colleagues (18) used transcriptome sequencing (RNA-Seq) to show that VanA-type vancomycin resistance genes are upregulated in Enterococcus faecium following exposure to CHX. In E. faecium, two genes encoding a two-component regulatory system were found to contribute to CHX tolerance (19). Thus, it is clear that Firmicutes have the capacity to develop increased tolerance to CHX, but the mechanisms by which tolerance may develop, especially in streptococci, are only beginning to be explored.…”

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confidence: 99%

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Spontaneously Arising Streptococcus mutans Variants with Reduced Susceptibility to Chlorhexidine Display Genetic Defects and Diminished Fitness

Kaspar

Godwin

Velsko

et al. 2019

Antimicrob Agents Chemother

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Chlorhexidine (CHX) has been used to control dental caries caused by acid-tolerant bacteria such as Streptococcus mutans since the 1970s. Repeat CHX exposure for other bacterial species results in the development of variants with reduced susceptibility that also become more resistant to other antimicrobials. It has not been tested if such variants arise when streptococci are exposed to CHX. Here, we passaged S. mutans in increasing concentrations of CHX and isolated spontaneously arising reduced susceptibility variants (RSVs) from separate lineages that have MICs that are up to 3-fold greater than the parental strain. The RSVs have increased growth rates at neutral pH and under acidic conditions in the presence of CHX but accumulate less biomass in biofilms. RSVs display higher MICs for daptomycin and clindamycin but increased sensitivity to dental-relevant antimicrobials triclosan and sodium fluoride. Plate-based assays for competition with health-associated oral streptococci revealed decreased bacteriocin production by the RSVs, increased sensitivity to hydrogen peroxide, and diminished competitive fitness in a human-derived ex vivo biofilm consortium. Whole-genome sequencing identified common single nucleotide polymorphisms (SNPs) within a diacylglycerol kinase homolog and a glycolipid synthesis enzyme, which could alter the accumulation of lipoteichoic acids and other envelope constituents, as well as a variety of mutations in other genes. Collectively, these findings confirm that S. mutans and likely other streptococci can develop tolerance to CHX but that increased tolerance comes at a fitness cost, such that CHX-induced variants that spontaneously arise in the human oral cavity may not persist.

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confidence: 99%

Spontaneously Arising Streptococcus mutans Variants with Reduced Susceptibility to Chlorhexidine Display Genetic Defects and Diminished Fitness

Kaspar

Godwin

Velsko

et al. 2019

Antimicrob Agents Chemother

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“…The two main mechanisms include CHX efflux (23, 42-44, 64-67) and changes in outer membrane content (68, 69). The recently identified two-component system ChtRS contributes to CHX tolerance in E. faecium , presumably via regulation of expression of genes in its regulon, which is currently undefined (70). In this study, we have confirmed a role for the heterodimeric ABC transporter in CHX susceptibility in VREfm.…”

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confidence: 99%

Reduced chlorhexidine and daptomycin susceptibility arises in vancomycin-resistantEnterococcus faeciumafter serial chlorhexidine exposure

Bhardwaj¹,

Hans²,

Ruikar³

et al. 2017

Preprint

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Vancomycin-resistant Enterococcus faecium (VREfm) are critical public health concerns because they are among the leading causes of hospital-acquired bloodstream infections. Chlorhexidine (CHX) is a bisbiguanide cationic antiseptic that is routinely used for patient bathing and other infection control practices. VREfm are likely frequently exposed to CHX; however, the long-term effects of CHX exposure have not been studied in enterococci. In this study, we serially exposed VREfm to increasing concentrations of CHX for a period of 21 days in two independent experimental evolution trials. Reduced CHX susceptibility emerged (4-fold shift in CHX MIC). Sub-populations with reduced daptomycin (DAP) susceptibility were detected, which were further analyzed by genome sequencing and lipidomic analysis. Across the trials, we identified adaptive changes in genes with predicted or experimentally confirmed roles in chlorhexidine susceptibility (efrE), global nutritional stress response (relA), nucleotide metabolism (cmk), phosphate acquisition (phoU), and glycolipid biosynthesis (bgsB), among others. Moreover, significant alterations in membrane phospholipids were identified. Our results are clinically significant because they identify a link between serial sub-inhibitory CHX exposure and reduced DAP susceptibility. In addition, the CHX-induced genetic and lipidomic changes described in this study offer new insights into the mechanisms underlying the emergence of antibiotic resistance in VREfm.

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“…However one recent study (6) reported that when CHX was continuously flowed on biofilms formed on polystyrene blocks in vitro, detached cells displayed a higher minimal inhibitory concentration (MIC) to CHX (1.25 μg mL −1 ), whereas most isolates of S. mutans evaluated had MICs < 1μg mL 1 . In enterococci, increased tolerance to antiseptics such as CHX in the hospital setting has inspired research into methods of increased CHX tolerance, including studies of CHX effects on the transcriptome (11) and on a transposon mutant library (12). More specifically, Bhardwaj and colleagues (11) used RNA-Seq to show that VanA-type vancomycin resistance genes are upregulated in Enterococcus faecium following CHX exposure.…”

Section: Introductionmentioning

confidence: 99%

“…More specifically, Bhardwaj and colleagues (11) used RNA-Seq to show that VanA-type vancomycin resistance genes are upregulated in Enterococcus faecium following CHX exposure. In E. faecium, two genes encoding for a two-component regulatory system were found to contribute to CHX tolerance (12). Thus, it is clear that Firmicutes have the capacity to develop increased tolerance to CHX, however the mechanisms by which tolerance may develop, especially in streptococci, is only beginning to be explored.…”

Section: Introductionmentioning

confidence: 99%

Characterization of Spontaneously Arising Chlorhexidine-Tolerant Variants inStreptococcus mutans

Kaspar

et al. 2019

Preprint

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22Broad spectrum antimicrobials, both in dental products and within the clinic, have been 23 used in the suppression of cariogenic bacteria such as Streptococcus mutans for over 40 years. 24One such antimicrobial is chlorhexidine (CHX), and serves as a standard in dental research 25 against which other antimicrobial therapies are compared against for their efficacy. However, 26 very little is known about the mode of action for CHX against Streptococci and whether 27 tolerance can be developed from repeated exposures. Here, we begin to answer such questions 28 by passaging S. mutans with increasing concentrations of CHX and isolating spontaneously-29 arising tolerant variants (CTVs) from separate lineages. We find that these CTVs display a 30 higher minimal inhibitory concentration (MIC) against CHX than the wild-type strain and have 31 altered virulence properties such as acid tolerance and biofilm formation. We record higher 32 MICs for the variants against both daptomycin and bacitracin, but find increased sensitivity to 33 triclosan and sodium fluoride. Measurements of antagonistic capabilities against other health-34 associated oral streptococci show decreased bacteriocin production compared to wild-type and 35 increased sensitivity to hydrogen peroxide. Finally whole genome sequencing of the CTVs show 36 common single nucleotide polymorphisms (SNPs) within a diacylglycerol kinase homolog and a 37 glycolipid synthesis enzyme, altering LTA accumulation and potentially lipid profile of the cell 38 wall. Together, these findings confirm that streptococci may develop tolerance to antimicrobial 39 agents such as CHX but in the case of S. mutans, increased tolerance may come at a fitness 40 cost for survival within oral biofilms that keeps variants suppressed within the population. 42 INTRODUCTION 43Controlling microbial biofilm infections in humans is challenging in part due to the 44 presence of extracellular polymeric substances (EPS) in which the organisms are embedded, 45 the presence of persister cells and sub-populations of cells with low metabolic activity, and 46 exchange of antimicrobial resistance genes through horizontal gene transfer. In the human oral 47 cavity, accumulation of biofilms on the teeth can lead to destruction of tooth mineral when there 48 is frequent and significant localized acidification by organic acids produced as metabolic end 49 products from fermentable carbohydrates (1). The initiation and progression of dental caries can 50 be controlled to a degree through non-specific mechanical removal of the biofilms or by 51 treatment with various chemical agents that include fluoride, xylitol or chlorhexidine (CHX) (2, 52 3). While the effectiveness of CHX in caries prevention is not definitively established and there 53 can be undesirable side effects (e.g. staining, irritation of host tissues) (4), CHX remains a 54 standard against which antimicrobial therapies are compared for their efficacy in the 55 suppression of caries-causing bacteria, such as Streptococcus mutans (5-7). Currently...

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The Two-Component System ChtRS Contributes to Chlorhexidine Tolerance in Enterococcus faecium

Cited by 33 publications

References 60 publications

Spontaneously Arising Streptococcus mutans Variants with Reduced Susceptibility to Chlorhexidine Display Genetic Defects and Diminished Fitness

Spontaneously Arising Streptococcus mutans Variants with Reduced Susceptibility to Chlorhexidine Display Genetic Defects and Diminished Fitness

Reduced chlorhexidine and daptomycin susceptibility arises in vancomycin-resistantEnterococcus faeciumafter serial chlorhexidine exposure

Characterization of Spontaneously Arising Chlorhexidine-Tolerant Variants inStreptococcus mutans

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