Affiliation:
1. W. M. Keck Center for Transgene Research, University of Notre Dame, Notre Dame, Indiana, USA
2. Department of Chemistry and Biochemistry, University of Notre Dame, Notre Dame, Indiana, USA
3. Department of Biological Sciences, University of Notre Dame, Notre Dame, Indiana, USA
Abstract
ABSTRACT
The genome of an invasive skin-tropic strain (AP53) of serotype M53 group A
Streptococcus pyogenes
(GAS) is composed of a circular chromosome of 1,860,554 bp and carries genetic markers for infection at skin locales,
viz
.,
emm
gene family pattern D and FCT type 3. Through genome-scale comparisons of AP53 with other GAS genomes, we identified 596 candidate single-nucleotide polymorphisms (SNPs) that reveal a potential genetic basis for skin tropism. The genome of AP53 differed by ∼30 point mutations from a noninvasive pattern D serotype M53 strain (Alab49), 4 of which are located in virulence genes. One pseudogene, yielding an inactive sensor kinase (CovS
−
) of the two-component transcriptional regulator CovRS, a major determinant for invasiveness, severely attenuated the expression of the secreted cysteine protease SpeB and enhanced the expression of the hyaluronic acid capsule compared to the isogenic noninvasive AP53/CovS
+
strain. The collagen-binding protein transcript
sclB
differed in the number of 5′-pentanucleotide repeats in the signal peptides of AP53 and Alab49 (9 versus 15), translating into different lengths of their signal peptides, which nonetheless maintained a full-length translatable coding frame. Furthermore, GAS strain AP53 acquired two phages that are absent in Alab49. One such phage (ΦAP53.2) contains the known virulence factor superantigen exotoxin gene tandem
speK-slaA
. Overall, we conclude that this bacterium has evolved in multiple ways, including mutational variations of regulatory genes, short-tandem-repeat polymorphisms, large-scale genomic alterations, and acquisition of phages, all of which may be involved in shaping the adaptation of GAS in specific infectious environments and contribute to its enhanced virulence.
IMPORTANCE
Infectious strains of
S. pyogenes
(GAS) are classified by their serotypes, relating to the surface M protein, the
emm
-like subfamily pattern, and their tropicity toward the nasopharynx and/or skin. It is generally agreed that M proteins from pattern D strains, which also directly bind human host plasminogen, are skin tropic. We have sequenced and characterized the genome of an invasive pattern D GAS strain (AP53) in comparison to a very similar strain (Alab49) that is noninvasive and developed a genomic rationale as to possible reasons for the skin tropicity of these two strains and the greater invasiveness of AP53.
Publisher
American Society for Microbiology
Subject
Molecular Biology,Microbiology