Characterization of Clinical and Carrier <i>Streptococcus agalactiae</i> and Prophage Contribution to the Strain Variability

• Main Authors: Aneta Lichvariková, Katarina Soltys, Tomas Szemes, Livia Slobodnikova, Gabriela Bukovska, Jan Turna, Hana Drahovska
• Format: Article
• Language: English
• Published: MDPI AG 2020-11-01
• Series: Viruses
• Subjects: <i>Streptococcus agalactiae</i>; MLST; prophage; WGS
• Online Access: https://www.mdpi.com/1999-4915/12/11/1323

<i>Streptococcus agalactiae</i> (group B Streptococcus, GBS) represents a leading cause of invasive bacterial infections in newborns and is also responsible for diseases in older and immunocompromised adults. Prophages represent an important factor contributing to the genome plasticity and evolution of new strains. In the present study, prophage content was analyzed in human GBS isolates. Thirty-seven prophages were identified in genomes of 20 representative sequenced strains. On the basis of the sequence comparison, we divided the prophages into eight groups named A–H. This division also corresponded to the clustering of phage integrase, even though several different integration sites were observed in some relative prophages. Next, PCR method was used for detection of the prophages in 123 GBS strains from adult hospitalized patients and from pregnancy screening. At least one prophage was present in 105 isolates (85%). The highest prevalence was observed for prophage group A (71%) and satellite prophage group B (62%). Other groups were detected infrequently (1–6%). Prophage distribution did not differ between clinical and screening strains, but it was unevenly distributed in MLST (multi locus sequence typing) sequence types. High content of full-length and satellite prophages detected in present study implies that prophages could be beneficial for the host bacterium and could contribute to evolution of more adapted strains.