Whole-Genome Comparison Uncovers Genomic Mutations between Group B Streptococci Sampled from Infected Newborns and Their Mothers

Almeida, Alexandre; Villain, Adrien; Joubrel, Caroline; Touak, Gérald; Sauvage, Elisabeth; Rosinski‐Chupin, Isabelle; Poyart, Claire; Glaser, Philippe

doi:10.1128/jb.00429-15

Cited by 23 publications

(20 citation statements)

References 70 publications

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“…Genetically divergent maternal-newborn dyads may reflect un-sampled variation in the mother, as only a single colony was sequenced in each case. Whilst adaptive mutations associated with disease progression have been reported elsewhere from the comparison of mother-newborn pairs,47 we were unable to find evidence for this in the current study, as all pairs involving invasive isolates were either genetically identical (0 SNVs), or divergent enough to argue against this. The findings show GBS infection occurs prior to delivery; supporting the need for IAP to be administered before delivery to be effective, and showing why antisepsis in active labour, for example vaginal chlorhexidine wipes, are ineffective in reducing neonatal EOD 8.…”

Section: Discussioncontrasting

confidence: 73%

Maternal colonization with Streptococcus agalactiae and associated stillbirth and neonatal disease in coastal Kenya

et al. 2016

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Streptococcus agalactiae (Group B Streptococcus, GBS) causes neonatal disease and stillbirth, but its burden in sub-Saharan Africa is uncertain. We assessed maternal recto-vaginal GBS colonisation (7967 women), stillbirth and neonatal disease. Whole genome sequencing was used to determine serotypes, sequence types (ST), and phylogeny. We found low maternal GBS colonisation prevalence (934/7967, 12%), but comparatively high incidence of GBS-associated stillbirth and early onset neonatal disease (EOD) in hospital (0.91(0.25-2.3)/1000 births; 0.76(0.25-1.77)/1000 live-births respectively). However, using a population denominator, EOD incidence was considerably reduced (0.13(0.07-0.21)/1000 live-births). Treated cases of EOD had very high case fatality (17/36, 47%), especially within 24 hours of birth, making under-ascertainment of community-born cases highly likely, both here and in similar facility-based studies. Maternal GBS colonisation was less common in women with low socio-economic status, HIV infection and undernutrition, but when GBS-colonised, they were more likely colonised by the most virulent clone, CC17. CC17 accounted for 267/915(29%) of maternal colonising (265/267(99%) serotype III, 2/267(0.7%) serotype IV), and 51/73(70%) of neonatal disease cases (all serotype III). Trivalent (Ia/II/III) and pentavalent (Ia/Ib/II/III/V) vaccines would cover 71/73(97%) and 72/73(99%) of disease-causing serotypes respectively. Serotype IV should be considered for inclusion, with evidence of capsular switching in CC17 strains.

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Section: Discussioncontrasting

confidence: 73%

Maternal colonization with Streptococcus agalactiae and associated stillbirth and neonatal disease in coastal Kenya

et al. 2016

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“…GBS strains lacking a functional CovR ( covR) cause significantly greater cytotoxicity in neutrophils compared to wildtype (WT) GBS and isogenic non-pigmented/non-hemolytic mutants due to enhanced production of Granadaene (Lamy et al, 2004;Jiang et al, 2005;Rajagopal et al, 2006;Boldenow et al, 2016). Furthermore, GBS strains lacking CovR have been identified and isolated from women in preterm labor (Whidbey et al, 2013) and from patients with other GBS infectious morbidities (Sendi et al, 2009;Lupo et al, 2014;Almeida et al, 2015Almeida et al, , 2017Whidbey et al, 2015a). We hypothesized that L. lactis pcylX-K, which lacks transcriptional repressors specific to the cyl operon, would induce neutrophil cytotoxicity similar to GBS covR.…”

Section: Resultsmentioning

confidence: 99%

The cyl Genes Reveal the Biosynthetic and Evolutionary Origins of the Group B Streptococcus Hemolytic Lipid, Granadaene

et al. 2020

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Group B Streptococcus (GBS) is a β-hemolytic, Gram-positive bacterium that commonly colonizes the female lower genital tract and is associated with fetal injury, preterm birth, spontaneous abortion, and neonatal infections. A major factor promoting GBS virulence is the β-hemolysin/cytolysin, which is cytotoxic to several host cells. We recently showed that the ornithine rhamnolipid pigment, Granadaene, produced by the gene products of the cyl operon, is hemolytic. Here, we demonstrate that heterologous expression of the GBS cyl operon conferred hemolysis, pigmentation, and cytoxicity to Lactococcus lactis, a model non-hemolytic Gram-positive bacterium. Similarly, pigment purified from L. lactis is hemolytic, cytolytic, and identical in structure to Granadaene extracted from GBS, indicating the cyl operon is sufficient for Granadaene production in a heterologous host. Using a systematic survey of phyletic patterns and contextual associations of the cyl genes, we identify homologs of the cyl operon in physiologically diverse Gram-positive bacteria and propose undescribed functions of cyl gene products. Together, these findings bring greater understanding to the biosynthesis and evolutionary foundations of a key GBS virulence factor and suggest that such potentially toxic lipids may be encoded by other bacteria.

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“…To obtain a detailed overview of the genomic diversity of CC17, we compiled all of the publicly available genomes belonging to CC17 as of May 2017 ( 8 , 15 , 17 – 20 ), together with a new panel of 45 strains, totaling a set of 626 GBS sequences (see Table S1 in the supplemental material). This comprises strains collected between 1955 and 2016 in Africa ( n = 359), Asia, ( n = 14), Europe ( n = 131), North America ( n = 95), and Australia ( n = 3), as well as others from unknown origins ( n = 24).…”

Section: Resultsmentioning

confidence: 99%

Parallel Evolution of Group B Streptococcus Hypervirulent Clonal Complex 17 Unveils New Pathoadaptive Mutations

et al. 2017

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The incidence of group B Streptococcus (GBS) neonatal disease continues to be a significant cause of concern worldwide. Strains belonging to clonal complex 17 (CC17) are the most frequently responsible for GBS infections in neonates, especially among late-onset disease cases. Therefore, we undertook the largest genomic study of GBS CC17 strains to date to decipher the genetic bases of their remarkable colonization and infection ability. We show that crucial functions involved in different steps of the colonization or infection process of GBS are distinctly mutated during the adaptation of CC17 to the human host. In particular, our results implicate the CovRS two-component regulator of virulence in the differentiation between carriage- and disease-associated isolates. Not only does this work raise important implications for the ongoing development of a vaccine against GBS but might also drive the discovery of key functions for GBS adaptation and pathogenesis that have been overlooked until now.

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Whole-Genome Comparison Uncovers Genomic Mutations between Group B Streptococci Sampled from Infected Newborns and Their Mothers

Cited by 23 publications

References 70 publications

Maternal colonization with Streptococcus agalactiae and associated stillbirth and neonatal disease in coastal Kenya

Maternal colonization with Streptococcus agalactiae and associated stillbirth and neonatal disease in coastal Kenya

The cyl Genes Reveal the Biosynthetic and Evolutionary Origins of the Group B Streptococcus Hemolytic Lipid, Granadaene

Parallel Evolution of Group B Streptococcus Hypervirulent Clonal Complex 17 Unveils New Pathoadaptive Mutations

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