Abstract
As a leading cause of neonatal sepsis, Streptococcus agalactiae, commonly known as Group B Streptococcus, is a major neonatal pathogen. Current global screening practices employ risk- or culture-based protocols for detection of these organisms. In Western Australia (WA), universal culture-based screening is provided, with subsequent intrapartum antibiotic prophylaxis for all S. agalactiae-positive women during labour. Widespread antibiotic exposure is not ideal and this is one of the factors driving development of vaccines against S. agalactiae. Vaccine candidates have focused on the capsule, surface proteins and pilus types, however, capsule serotypes are known to vary geographically. The aim of this study was to use genome sequencing to gain an understanding of the circulating genotypes in WA, and to assess variations in the associated gene pools. We sequenced 141 antenatal carriage (vaginal/rectal) isolates and 10 neonatal invasive disease isolates from WA. Based on the global PubMLST database, the 151 strains were characterised into 30 sequence types, with clustering of these mainly into clonal complexes 1, 12, 17, 19 and 23. Of the genes encoding eleven surface proteins that were analysed, the most prevalent were fbp, lmb and scpB which were present in ≥ 98% of isolates. A cluster of non-haemolytic isolates, one of which was a neonatal invasive disease isolate, appeared to lack the entire cyl locus. Admixture analysis of population structure revealed evidence of genetic transfer among the WA isolates across structural groups. When compared against the PubMLST S. agalactiae data, WA isolates showed high levels of strain diversity with minimal apparent clustering. This is the first whole genome sequence study of WA S. agalactiae isolates and also represents the first addition of Australian isolate data to PubMLST. This report provides insight into the distribution and diversity of vaccine targets of S. agalactiae within Western Australia, indicating that the most appropriate capsular vaccine for this population would be the proposed pentavalent (Cps Ia, Ib, II, III and V) preparation, whilst vaccines targeting surface proteins should ideally utilise Fbp, Lmb and/or ScpB.
Highlights
As an opportunistic pathogen, Streptococcus agalactiae, commonly known as Group B Streptococcus, is able to reside as a commensal in some individuals and cause serious infection in others; commonly those who are immunocompromised, and typically the elderly or neonates
Knowledge of capsule (CPS) serotype is of significant importance for formulating vaccines that target the S. agalactiae capsule, with the exception of CPS III, information on serotype is not useful for comparing carriage and invasive disease isolates which are generally found distributed amongst all serotypes [5]
The majority of the clinical isolates collected from Western Australia (WA) were observed to cluster into five clonal complexes (CCs), CC1, CC12, CC17, CC19 and CC23 (Fig 1A), a small cluster (n = 5) of ST22 isolates and a single ST248 isolate were observed
Summary
Streptococcus agalactiae, commonly known as Group B Streptococcus, is able to reside as a commensal in some individuals and cause serious infection in others; commonly those who are immunocompromised, and typically the elderly or neonates. Knowledge of capsule (CPS) serotype is of significant importance for formulating vaccines that target the S. agalactiae capsule, with the exception of CPS III, information on serotype is not useful for comparing carriage and invasive disease isolates which are generally found distributed amongst all serotypes [5]. This is further complicated by reports of capsular switching [6,7,8,9] and discrepant results between serotyping methods [10,11]
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