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  4. Influence of Staphylococcus aureus Strain Background on Sa3int Phage Life Cycle Switches
 
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2022
Journal Article
Title

Influence of Staphylococcus aureus Strain Background on Sa3int Phage Life Cycle Switches

Abstract
Staphylococcus aureus asymptomatically colonizes the nasal cavity of mammals, but it is also a leading cause of life-threatening infections. Most human nasal isolates carry Sa3 phages, which integrate into the bacterial hlb gene encoding a sphingomyelinase. The virulence factor-encoding genes carried by the Sa3-phages are highly human-specific, and most animal strains are Sa3 negative. Thus, both insertion and excision of the prophage could potentially confer a fitness advantage to S. aureus. Here, we analyzed the phage life cycle of two Sa3 phages, Φ13 and ΦN315, in different phage-cured S. aureus strains. Based on phage transfer experiments, strains could be classified into low (8325-4, SH1000, and USA300c) and high (MW2c and Newman-c) transfer strains. High-transfer strains promoted the replication of phages, whereas phage adsorption, integration, excision, or recA transcription was not significantly different between strains. RNASeq analyses of replication-deficient lysogens revealed no strain-specific differences in the CI/Mor regulatory switch. However, lytic genes were significantly upregulated in the high transfer strain MW2c Φ13 compared to strain 8325-4 Φ13. By transcriptional start site prediction, new promoter regions within the lytic modules were identified, which are likely targeted by specific host factors. Such host-phage interaction probably accounts for the strain-specific differences in phage replication and transfer frequency. Thus, the genetic makeup of the host strains may determine the rate of phage mobilization, a feature that might impact the speed at which certain strains can achieve host adaptation.
Author(s)
Rohmer, Carina
Fraunhofer-Institut für Grenzflächen- und Bioverfahrenstechnik IGB  
Dobritz, Ronja
Tuncbilek-Dere, Dilek
Lehmann, Esther
Gerlach, David
George, Shilpa Elizabeth
Bae, Taeok
Nieselt, Kay
Wolz, Christiane
Journal
Viruses  
Open Access
DOI
10.3390/v14112471
Language
English
Fraunhofer-Institut für Grenzflächen- und Bioverfahrenstechnik IGB  
Keyword(s)
  • gene regulation

  • hemolysin

  • induction

  • phage

  • Staphylococcus

  • virulence

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