Abstract

The major human pathogen Streptococcus pyogenes shares an intimate evolutionary history with mobile genetic elements, which in many cases carry genes encoding bacterial virulence factors. During recent whole-genome sequencing of a longitudinal sample of S. pyogenes isolates in England, we identified a lineage within emm4 that clustered with the reference genome MEW427. Like MEW427, this lineage was characterized by substantial gene loss within all three prophage regions, compared to MGAS10750 and isolates outside of the MEW427-like lineage. Gene loss primarily affected lysogeny, replicative and regulatory modules, and to a lesser and more variable extent, structural genes. Importantly, prophage-encoded superantigen and DNase genes were retained in all isolates. In isolates where the prophage elements were complete, like MGAS10750, they could be induced experimentally, but not in MEW427-like isolates with degraded prophages. We also found gene loss within the chromosomal island SpyCIM4 of MEW427-like isolates, although surprisingly, the SpyCIM4 element could not be experimentally induced in either MGAS10750-like or MEW427-like isolates. This did not, however, appear to abolish expression of the mismatch repair operon, within which this element resides. The inclusion of further emm4 genomes in our analyses ratified our observations and revealed an international emm4 lineage characterized by prophage degradation. Intriguingly, the USA population of emm4 S. pyogenes appeared to constitute predominantly MEW427-like isolates, whereas the UK population comprised both MEW427-like and MGAS10750-like isolates. The degraded and cryptic nature of these elements may have important phenotypic and fitness ramifications for emm4 S. pyogenes , and the geographical distribution of this lineage raises interesting questions on the population dynamics of the genotype.

Highlights

  • IntroductionStreptococcus pyogenes ( known as the Lancefield group A Streptococcus or GAS) is a globally distributed human pathogen [1]

  • Streptococcus pyogenes is a globally distributed human pathogen [1]

  • We have identified a lineage within an international emm4 population that is characterized by degradation within integrated prophage genomes

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Summary

Introduction

Streptococcus pyogenes ( known as the Lancefield group A Streptococcus or GAS) is a globally distributed human pathogen [1]. The spectrum of infections caused by S. pyogenes is broad, with manifestations ranging from the relatively mild and self-limiting tonsillitis and scarlet fever, to the more severe, invasive and potentially life-threatening, notably necrotizing fasciitis and streptococcal toxic shock syndrome [2]. S. pyogenes isolates are classified into emm genotypes in accordance with the 5′ hypervariable region of the emm gene, which encodes the surface protein M [3, 4]. Most S. pyogenes genotypes are lysogenized by at least one prophage, though it is not at all uncommon for certain. There is, a general lack of knowledge regarding prophages and phage-like elements and their impact on streptococcal biology, despite their prevalence

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