The Thymidine-Dependent Small-Colony-Variant Phenotype Is Associated with Hypermutability and Antibiotic Resistance in Clinical
            <i>Staphylococcus aureus</i>
            Isolates

Besier, Silke; Zander, Johannes; Kahl, Barbara C.; Kraiczy, Peter; Brade, Volker; Wichelhaus, Thomas A.

doi:10.1128/aac.01395-07

Cited by 75 publications

(72 citation statements)

References 48 publications

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“…S. aureus persists in the airways of people with CF for years and can develop a hypermutator phenotype that promotes adaptive changes, including SCVs, thought to facilitate survival of this organism within the CF airway. 84,85 SCVs are detected visually on laboratory agar plates and exhibit slower growth rates due to metabolic defects (eg, thymidine biosynthesis deficiency 86 ), and they therefore require special susceptibility testing. However, the testing method has not been standardized by the Clinical and Laboratory Standards Institute.…”

Section: Ic4 Small Colony Variant (Scv) S Aureusmentioning

confidence: 99%

“…SCV strains of S. aureus are thought to have increased resistance to the innate immune system and increased resistance to antibiotics. 85,87,88 In vitro, SCVs have an increased ability to infect normal and CF airway epithelial cells. 89 In non-CF patients, SCV S. aureus are associated with chronic or recurrent infections, such as endocarditis and osteomyelitis.…”

Section: Ic4 Small Colony Variant (Scv) S Aureusmentioning

confidence: 99%

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Infection Prevention and Control Guideline for Cystic Fibrosis: 2013 Update

Saiman

Siegel

LiPuma

et al. 2014

Infect. Control Hosp. Epidemiol.

352

382

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The 2013 Infection Prevention and Control (IP&C) Guideline for Cystic Fibrosis (CF) was commissioned by the CF Foundation as an update of the 2003 Infection Control Guideline for CF. During the past decade, new knowledge and new challenges provided the following rationale to develop updated IP&C strategies for this unique population:1. The need to integrate relevant recommendations from evidence-based guidelines published since 2003 into IP&C practices for CF. These included guidelines from the Centers for Disease Control and Prevention (CDC)/Healthcare Infection Control Practices Advisory Committee (HICPAC), the World Health Organization (WHO), and key professional societies, including the Infectious Diseases Society of America (IDSA) and the Society for Healthcare Epidemiology of America (SHEA). During the past decade, new evidence has led to a renewed emphasis on source containment of potential pathogens and the role played by the contaminated healthcare environment in the transmission of infectious agents. Furthermore, an increased understanding of the importance of the application of implementation science, monitoring adherence, and feedback principles has been shown to increase the effectiveness of IP&C guideline recommendations.2. Experience with emerging pathogens in the non-CF population has expanded our understanding of droplet transmission of respiratory pathogens and can inform IP&C strategies for CF. These pathogens include severe acute respiratory syndrome coronavirus and the 2009 influenza A H1N1. Lessons learned about preventing transmission of methicillin-resistant Staphylococcus aureus (MRSA) and multidrug-resistant gram-negative pathogens in non-CF patient populations also can inform IP&C strategies for CF.

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Section: Ic4 Small Colony Variant (Scv) S Aureusmentioning

confidence: 99%

Section: Ic4 Small Colony Variant (Scv) S Aureusmentioning

confidence: 99%

Infection Prevention and Control Guideline for Cystic Fibrosis: 2013 Update

Saiman

Siegel

LiPuma

et al. 2014

Infect. Control Hosp. Epidemiol.

352

382

View full text Add to dashboard Cite

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“…For example, thymidine-dependent smallcolony variants of Staphylococcus aureus, which are frequently isolated in CF patients and are implicated in persistent and recurrent infections, are hypermutators (Besier et al, 2008). Inactivation of the MMR system favours long-term persistence of oropharyngeal colonization by P. aeruginosa in CF mice .…”

Section: Clinical Implications Of Hypermutator Strainsmentioning

confidence: 99%

Bacterial hypermutation: clinical implications

Jolivet‐Gougeon

Kovács

Gall‐David

et al. 2011

Journal of Medical Microbiology

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Heritable hypermutation in bacteria is mainly due to alterations in the methyl-directed mismatch repair (MMR) system. MMR-deficient strains have been described from several bacterial species, and all of the strains exhibit increased mutation frequency and recombination, which are important mechanisms for acquired drug resistance in bacteria. Antibiotics select for drug-resistant strains and refine resistance determinants on plasmids, thus stimulating DNA recombination via the MMR system. Antibiotics can also act as indirect promoters of antibiotic resistance by inducing the SOS system and certain error-prone DNA polymerases. These alterations have clinical consequences in that efficacious treatment of bacterial infections requires high doses of antibiotics and/or a combination of different classes of antimicrobial agents. There are currently few new drugs with low endogenous resistance potential, and the development of such drugs merits further research. IntroductionEradication of infectious diseases is constantly challenged by micro-organisms that develop new survival strategies. Previous studies suggest that mutational events play a predominant role in bacterial adaptation and confer a selective advantage (Chou et al., 2009;Cooper, 2007). Early experiments aimed at detecting mutators used mutagenized laboratory strains of bacteria, sometimes coupled with different selection strategies. LeClerc et al. (1996) reported high mutation frequency among Escherichia coli and Salmonella pathogens, challenging the theory that mutators were rare among bacterial populations. Taken together, these findings demonstrated that natural populations could respond to environmental selection in two ways, i.e. by enhanced mutation frequencies and by recombination. Transient mutator status, which involves reversion or recombination within the mutator alleles or depletion of the methyl-directed mismatch repair (MMR) system proteins, allows the organism to temporarily benefit from the elevated mutation frequency for adaptation while reducing the risk of accumulating deleterious mutations. Using a mathematical model, Rosche & Foster (1999) showed that transient hypermutators play a role in adaptive mutation in E. coli. Molecular mechanisms of hypermutationProteins involved in the DNA mismatch repair pathway help replace nucleotides introduced erroneously into the replicated DNA and also hinder recombination between non-identical DNA sequences. Deficiencies in any of the DNA mismatch repair pathway mechanisms can lead to a hypermutator phenotype. DNA repairSiegel & Bryson (1967) discovered the mutS gene in an azaserine-resistant derivative of E. coli that had a mutator phenotype and carried a deletion in the mutS gene. The majority of naturally occurring strong mutators have defects in the MMR system; the mutations are mainly in mutS (Oliver et al., 2002), but deletions in genes encoding beta-clamp proteins and in mutH, mutL and mutU (uvrD) have also been described (Fig. 1). Inactivation of basal excision repair genes, e.g. mutY, mutM, ...

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“…Antimicrobial susceptibility was tested by Etest (bioMérieux, Marcy l'Etoile, France) by following the manufacturer's instructions (except that 5% defibrinated sheep blood was added to the medium, as previously described [5,6]) for all tested antimicrobics except gentamicin, amikacin, tobramycin, and kanamycin, which were tested by agar dilution following Clinical and Laboratory Standards Institutes guidelines (10) (except that 5% defibrinated sheep blood was added to the media, as previously described [5,6]). All testing was simultaneously performed on control strain S. aureus ATCC 29213 and was within the quality control range specified by Clinical and Laboratory Standards Institutes guidelines (11).…”

mentioning

confidence: 99%

“…Thymidine auxotrophs are thought to arise due to antibiotic pressure after prolonged exposure to TMP-SMX (6,7). This has been best described in isolates from the airways of cystic fibrosis patients on chronic TMP-SMX therapy (15,17), but long-term TMP-SMX has also been associated with thymidine auxotrophy in S. aureus isolates from patients without cystic fibrosis (7).…”

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confidence: 99%

Thymidine Auxotrophic Staphylococcus aureus Small-Colony Variant Endocarditis and Left Ventricular Assist Device Infection

et al. 2012

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We describe a thymidine-dependent small-colony variant of Staphylococcus aureus associated with left ventricular assist device infection and prosthetic valve and pacemaker endocarditis. CASE REPORTT he patient was a 34-year-old woman who 3 years prior had suffered an anterior wall myocardial infarction resulting in ischemic cardiomyopathy, which necessitated placement of a pacemaker biventricular defibrillator. Subsequently, there was progressive deterioration of cardiac function. A left ventricular assist device (LVAD) was placed as a bridge to heart transplantation. During the same surgery, her native tricuspid valve was replaced with a pericardial tissue valve on account of tricuspid regurgitation. One month after surgery, she developed fever and chills, and blood cultures grew methicillin-resistant Staphylococcus aureus (MRSA) which was susceptible to gentamicin, rifampin, linezolid, trimethoprim-sulfamethoxazole (TMP-SMX), and vancomycin (MIC, 2 g/ml) and resistant to erythromycin and levofloxacin. Trans-esophageal echocardiography (TEE) showed no evidence of endocarditis. She was treated with 6 weeks of vancomycin and rifampin, with gentamicin administered during the first 2 weeks of therapy. Five days after completing antimicrobial therapy, she developed recurrent fevers, and blood cultures again grew MRSA which was susceptible to gentamicin, linezolid, TMP-SMX, vancomycin (MIC, 1 g/ml), and daptomycin and resistant to rifampin, erythromycin, and levofloxacin. A TEE demonstrated vegetations on the pacemaker leads and the prosthetic tricuspid valve. She was treated with daptomycin, gentamicin, and (until the isolate was known to be resistant to rifampin) rifampin. A follow-up TEE after 2 months of antimicrobial therapy showed reduction in the size of the vegetations. She received 5 months of daptomycin and gentamicin; TEE at the end of therapy showed old and healed vegetations. However, over the ensuing year, she had recurrent MRSA bacteremia and soft tissue infection surrounding her LVAD generator site. As a result, from December 2008 through March 2010, she received continuous antimicrobial therapy with various combinations of vancomycin, rifampin, daptomycin, gentamicin, quinupristin-dalfopristin, and TMP-SMX (Fig. 1). During this time, only one isolate (of several) was identifiable, and susceptibility testing was reportable using the BD Phoenix automated microbiology system (BD Diagnostic Systems, Franklin Lakes, NJ). That isolate, recovered from an umbilical driveline aspirate, was reported as susceptible to gentamicin, linezolid, TMP-SMX, and vancomycin (MIC, 2 g/ml), resistant to rifampin, erythromycin, and levofloxacin, and nonsusceptible to daptomycin (MIC, 4 g/ml). Because of inadequate growth in the test medium, other isolates, including bloodstream isolates and another umbilical driveline aspirate, were not identifiable, and susceptibility testing was not reportable using the BD Phoenix automated microbiology system.Despite ongoing combination antimicrobial therapy and incision and drainage of ...

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The Thymidine-Dependent Small-Colony-Variant Phenotype Is Associated with Hypermutability and Antibiotic Resistance in Clinical Staphylococcus aureus Isolates

Cited by 75 publications

References 48 publications

Infection Prevention and Control Guideline for Cystic Fibrosis: 2013 Update

Infection Prevention and Control Guideline for Cystic Fibrosis: 2013 Update

Bacterial hypermutation: clinical implications

Thymidine Auxotrophic Staphylococcus aureus Small-Colony Variant Endocarditis and Left Ventricular Assist Device Infection

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