A Genomic Virulence Reference Map of Enterococcus faecalis Reveals an Important Contribution of Phage03-Like Elements in Nosocomial Genetic Lineages to Pathogenicity in a Caenorhabditis elegans Infection Model

Rosa, Sabina Leanti La; Snipen, Lars; Murray, Barbara E.; Willems, Rob J. L.; Gilmore, Michael S.; Diep, Dzung B.; Nes, Ingolf F.; Brede, Dag Anders

doi:10.1128/iai.02801-14

Cited by 15 publications

(15 citation statements)

References 66 publications

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“…As mentioned above the population structure of E. faecalis seems to be significantly different from E. faecium as no clearly defined E. faecalis ecotypes appear to exist. Correspondingly, previous studies have reported shared antibiotic resistance and virulence genes, such as the E. faecalis pathogenicity island, esp , capsule polysaccharide genes, and genes encoding for gelatinase, aggregation substance, cytolysin, and Ace, among E. faecalis isolates from a wide variety of different niches like the hospital, animals, food products and the environment ( Eaton and Gasson, 2001 ; Creti et al, 2004 ; McBride et al, 2007 ; Freitas et al, 2009 ; Solheim et al, 2009 ; La Rosa et al, 2015 ). Note that the absence of clearly defined ecotypes in E. faecalis can be interpreted as a high multiplicity of closely related fine-grained ecotypes, none of them reaching predominance.…”

Section: Adaptive Elements In Nosocomial Lineagesmentioning

confidence: 77%

Global Emergence and Dissemination of Enterococci as Nosocomial Pathogens: Attack of the Clones?

et al. 2016

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Enterococci are Gram-positive bacteria that are found in plants, soil and as commensals of the gastrointestinal tract of humans, mammals, and insects. Despite their commensal nature, they have also become globally important nosocomial pathogens. Within the genus Enterococcus, Enterococcus faecium, and Enterococcus faecalis are clinically most relevant. In this review, we will discuss how E. faecium and E. faecalis have evolved to become a globally disseminated nosocomial pathogen. E. faecium has a defined sub-population that is associated with hospitalized patients and is rarely encountered in community settings. These hospital-associated clones are characterized by the acquisition of adaptive genetic elements, including genes involved in metabolism, biofilm formation, and antibiotic resistance. In contrast to E. faecium, clones of E. faecalis isolated from hospitalized patients, including strains causing clinical infections, are not exclusively found in hospitals but are also present in healthy individuals and animals. This observation suggests that the division between commensals and hospital-adapted lineages is less clear for E. faecalis than for E. faecium. In addition, genes that are reported to be associated with virulence of E. faecalis are often not unique to clinical isolates, but are also found in strains that originate from commensal niches. As a reflection of more ancient association of E. faecalis with different hosts, these determinants Thus, they may not represent genuine virulence genes but may act as host-adaptive functions that are useful in a variety of intestinal environments. The scope of the review is to summarize recent trends in the emergence of antibiotic resistance and explore recent developments in the molecular epidemiology, population structure and mechanisms of adaptation of E. faecium and E. faecalis.

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Section: Adaptive Elements In Nosocomial Lineagesmentioning

confidence: 77%

Global Emergence and Dissemination of Enterococci as Nosocomial Pathogens: Attack of the Clones?

et al. 2016

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“…Intact or relics of prophages highly identical to sequences from common enterococcal prophages such as phiL1A and vB_IME197 were identified in most strains, but the exact phage(s) present in each genome cannot be ruled out with accuracy. The phiL1A and vB_IME197 phages are widespread in E. faecalis from variable sources [31] and were originally described in clinical settings in UK and China, respectively [54,55] [58]. In this study, this phage was putatively identified in three related ST476 strains from hospitalized patients, farm and retail chicken in China and Tunisia (Table S6), once more enphasizing the lack of a demarcation between clinical and non-clinical genomes in relevant mobile genetic elements (MGEs).…”

Section: Prophagesmentioning

confidence: 85%

Comparative genomics of global optrA-carrying Enterococcus faecalis uncovers a common chromosomal hotspot for optrA acquisition within a diversity of core and accessory genomes

et al. 2020

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Linezolid-resistant Enterococcus faecalis (LREfs) carrying optrA are increasingly reported globally from multiple sources, but we lack a comprehensive analysis of human and animal optrA-LREfs strains. To assess if optrA is dispersed in isolates with varied genetic backgrounds or with common genetic features, we investigated the phylogenetic structure, genetic content [antimicrobial resistance (AMR), virulence, prophages, plasmidome] and optrA-containing platforms of 27 publicly available optrA-positive E. faecalis genomes from different hosts in seven countries. At the genome-level analysis, an in-house database with 64 virulence genes was tested for the first time. Our analysis showed a diversity of clones and adaptive gene sequences related to a wide range of genera from Firmicutes . Phylogenies of core and accessory genomes were not congruent, and at least PAI-associated and prophage genes contribute to such differences. Epidemiologically unrelated clones (ST21, ST476-like and ST489) obtained from human clinical and animal hosts in different continents over eight years (2010–2017) could be phylogenetically related (3–126 SNPs difference). optrA was located on the chromosome within a Tn6674-like element (n=10) or on medium-size plasmids (30–60 kb; n=14) belonging to main plasmid families (RepA_N/Inc18/Rep_3). In most cases, the immediate gene vicinity of optrA was generally identical in chromosomal (Tn6674) or plasmid (impB-fexA-optrA) backbones. Tn6674 was always inserted into the same ∆radC integration site and embedded in a 32 kb chromosomal platform common to strains from different origins (patients, healthy humans, and animals) in Europe, Africa, and Asia during 2012–2017. This platform is conserved among hundreds of E. faecalis genomes and proposed as a chromosomal hotspot for optrA integration. The finding of optrA in strains sharing common adaptive features and genetic backgrounds across different hosts and countries suggests the occurrence of common and independent genetic events occurring in distant regions and might explain the easy de novo generation of optrA-positive strains. It also anticipates a dramatic increase of optrA carriage and spread with a serious impact on the efficacy of linezolid for the treatment of Gram-positive infections.

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“…Many studies of enterococcal virulence and pathogenesis have understandably focused on gene products encoded by mobile elements identified in clinical isolates from infections ( 7 , 8 ). In contrast, we and others have identified loci within the conserved core genome that are also required for virulence ( 9 – 14 ).…”

Section: Introductionmentioning

confidence: 99%

Comprehensive Functional Analysis of the Enterococcus faecalis Core Genome Using an Ordered, Sequence-Defined Collection of Insertional Mutations in Strain OG1RF

et al. 2018

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The robust ability of Enterococcus faecalis to survive outside the host and to spread via oral-fecal transmission and its high degree of intrinsic and acquired antimicrobial resistance all complicate the treatment of hospital-acquired enterococcal infections. The conserved E. faecalis core genome serves as an important genetic scaffold for evolution of this bacterium in the modern health care setting and also provides interesting vaccine and drug targets. We used an innovative pooling/sequencing strategy to map a large collection of arrayed transposon insertions in E. faecalis OG1RF and generated an arrayed library of defined mutants covering approximately 70% of the OG1RF genome. Then, we performed high-throughput transposon sequencing experiments using this library to determine core genomic determinants of bile resistance in OG1RF. This collection is a valuable resource for comprehensive, functional enterococcal genomics using both traditional and high-throughput approaches and enables immediate recovery of mutants of interest.

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A Genomic Virulence Reference Map of Enterococcus faecalis Reveals an Important Contribution of Phage03-Like Elements in Nosocomial Genetic Lineages to Pathogenicity in a Caenorhabditis elegans Infection Model

Cited by 15 publications

References 66 publications

Global Emergence and Dissemination of Enterococci as Nosocomial Pathogens: Attack of the Clones?

Global Emergence and Dissemination of Enterococci as Nosocomial Pathogens: Attack of the Clones?

Comparative genomics of global optrA-carrying Enterococcus faecalis uncovers a common chromosomal hotspot for optrA acquisition within a diversity of core and accessory genomes

Comprehensive Functional Analysis of the Enterococcus faecalis Core Genome Using an Ordered, Sequence-Defined Collection of Insertional Mutations in Strain OG1RF

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