Streptococcus agalactiae clones infecting humans were selected and fixed through the extensive use of tetracycline

Cunha, Violette Da; Davies, Mark R.; Douarre, Pierre E.; Rosinski‐Chupin, Isabelle; Margarit, Immaculada; Spinali, Sebastien; Perkins, Tim; Lechat, Pierre; Dmytruk, Nicolas; Sauvage, Elisabeth; Ma, Laurence; Romi, Benedetta; Tichit, Magali; López‐Sánchez, María José; Descorps-Declère, Stéphane; Souche, Erika; Buchrieser, Carmen; Trieu-Cuot, Patrick; Moszer, Ivan; Clermont, Dominique; Maione, Domenico; Bouchier, Christiane; McMillan, David; Parkhill, Julian; Telford, John L.; Dougan, Gordan; Walker, Mark J.; Holden, Matthew T. G.; Poyart, Claire; Glaser, Philippe

doi:10.1038/ncomms5544

Cited by 210 publications

(285 citation statements)

References 58 publications

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“…Macrolide resistance factors were present at a relatively higher rate in the present study (59%; SI Appendix, Fig. S5A) than what has been reported in other GBS studies (10,17). The majority of macrolide resistance elements were ermB or ermTR (SI Appendix, Fig.…”

Section: High Rates Of Antimicrobial Resistance Genes Present In St-1contrasting

confidence: 54%

“…When present, tetM was invariably located in the transposable element Tn916 inserted in RDF.2 (SI Appendix, Fig. S1) at the location reported for the Tn916-1 lineage by Da Cunha et al (10). Macrolide resistance factors were present at a relatively higher rate in the present study (59%; SI Appendix, Fig.…”

Section: High Rates Of Antimicrobial Resistance Genes Present In St-1mentioning

confidence: 43%

“…S3D). We additionally analyzed 24 serotype V ST-1 strains from three different continents and for which whole-genome data were recently reported (10) and found that the strains were interspersed among our North American isolates, suggesting the global dissemination of the ST-1 clone (SI Appendix, Fig. S4).…”

Section: Genetic Relationship Among St-1 Gbs Strains Lacking Evidence Ofmentioning

confidence: 99%

“…GBS is divided into 10 serotypes based on the carbohydrate composition of its sialic acid containing capsule, but gene content at the genomic level does not necessarily correlate with capsular serotype (8,9). A seven-gene multilocus sequence typing (MLST) allows for the classification of the majority of GBS strains isolated from humans into five major clonal complexes (CCs) with a recent study by Da Cunha et al showing that the major GBS CCs are primarily derived from a limited number of tetracycline-resistant clones, suggesting a key role of tetracycline resistance in GBS strain emergence (10,11). CC-17 GBS strains have been particularly well studied given their role as the major cause of severe, invasive infant disease (10,12).…”

mentioning

confidence: 99%

“…A seven-gene multilocus sequence typing (MLST) allows for the classification of the majority of GBS strains isolated from humans into five major clonal complexes (CCs) with a recent study by Da Cunha et al showing that the major GBS CCs are primarily derived from a limited number of tetracycline-resistant clones, suggesting a key role of tetracycline resistance in GBS strain emergence (10,11). CC-17 GBS strains have been particularly well studied given their role as the major cause of severe, invasive infant disease (10,12). In contrast, serotype V strains cause a larger percentage of invasive disease in nonpregnant adults compared with neonates (13)(14)(15).…”

mentioning

confidence: 99%

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Sequence type 1 group B Streptococcus , an emerging cause of invasive disease in adults, evolves by small genetic changes

Galloway-Peña

Sahasrabhojane

Saldaña

et al. 2015

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

101

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The molecular mechanisms underlying pathogen emergence in humans is a critical but poorly understood area of microbiologic investigation. Serotype V group B Streptococcus (GBS) was first isolated from humans in 1975, and rates of invasive serotype V GBS disease significantly increased starting in the early 1990s. We found that 210 of 229 serotype V GBS strains (92%) isolated from the bloodstream of nonpregnant adults in the United States and Canada between 1992 and 2013 were multilocus sequence type (ST) 1. Elucidation of the complete genome of a 1992 ST-1 strain revealed that this strain had the highest homology with a GBS strain causing cow mastitis and that the 1992 ST-1 strain differed from serotype V strains isolated in the late 1970s by acquisition of cell surface proteins and antimicrobial resistance determinants. Whole-genome comparison of 202 invasive ST-1 strains detected significant recombination in only eight strains. The remaining 194 strains differed by an average of 97 SNPs. Phylogenetic analysis revealed a temporally dependent mode of genetic diversification consistent with the emergence in the 1990s of ST-1 GBS as major agents of human disease. Thirty-one loci were identified as being under positive selective pressure, and mutations at loci encoding polysaccharide capsule production proteins, regulators of pilus expression, and two-component gene regulatory systems were shown to affect the bacterial phenotype. These data reveal that phenotypic diversity among ST-1 GBS is mainly driven by small genetic changes rather than extensive recombination, thereby extending knowledge into how pathogens adapt to humans.Streptococcus agalactiae | pathogenesis | evolution | single nucleotide polymorphisms | surface protein

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Section: High Rates Of Antimicrobial Resistance Genes Present In St-1contrasting

confidence: 54%

Section: High Rates Of Antimicrobial Resistance Genes Present In St-1mentioning

confidence: 43%

Section: Genetic Relationship Among St-1 Gbs Strains Lacking Evidence Ofmentioning

confidence: 99%

mentioning

confidence: 99%

mentioning

confidence: 99%

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Sequence type 1 group B Streptococcus , an emerging cause of invasive disease in adults, evolves by small genetic changes

Galloway-Peña

Sahasrabhojane

Saldaña

et al. 2015

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

101

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The role of CNS macrophages in streptococcal meningoencephalitis

Gres

Kolter

Erny

et al. 2019

Journal of Leukocyte Biology

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In the healthy brain, microglia and other CNS macrophages are the most abundant immune cell type. Thus, they form the natural immune cell interface with streptococci, which are the leading cause of bacterial meningitis and encephalitis in infants and young children. In homeostasis, the blood-brain barrier allows for very limited access of immune cells circulating in the periphery. During bacterial meningoencephalitis, however, origin and fate of CNS macrophages are massively altered. This review summarizes the emerging knowledge on the sequence of reciprocal events between streptococci and CNS macrophages leading to host resistance, acute inflammation, changes in resident innate immune cells of the brain, and long-term neuronal damage. K E Y W O R D S meningitis, microglia, Streptococcus agalactiae, Streptococcus pneumoniae [The copyright line for this article was changed on 25 February 2019 after original online publication] of events can transiently severely perturb the separation of the CNS and the peripheral immune system. Thereby, long-term consequences for neurodevelopment might ensue.

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Streptococcus agalactiae (Group B Streptococcus)

Shabayek

2022

Molecular Typing in Bacterial Infections, Volume I

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Streptococcus agalactiae clones infecting humans were selected and fixed through the extensive use of tetracycline

Cited by 210 publications

References 58 publications

Sequence type 1 group B Streptococcus , an emerging cause of invasive disease in adults, evolves by small genetic changes

Sequence type 1 group B Streptococcus , an emerging cause of invasive disease in adults, evolves by small genetic changes

The role of CNS macrophages in streptococcal meningoencephalitis

Streptococcus agalactiae (Group B Streptococcus)

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