Characterization of emergent toxigenic M1(UK) Streptococcus pyogenes and associated sublineages

Streptococcus pyogenes genotype emm1 is a successful, globally distributed epidemic clone that is regarded as inherently virulent. An emm1 sublineage, M1(UK), that produces increased levels of SpeA toxin was associated with increased scarlet fever and invasive infections in England in 2015/2016. Def...

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Detalles Bibliográficos
Autores principales: Li, Ho Kwong, Zhi, Xiangyun, Vieira, Ana, Whitwell, Harry J., Schricker, Amelia, Jauneikaite, Elita, Li, Hanqi, Yosef, Ahmed, Andrew, Ivan, Game, Laurence, Turner, Claire E., Lamagni, Theresa, Coelho, Juliana, Sriskandan, Shiranee
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Microbiology Society 2023
Materias:
Research Articles
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10210942/
https://www.ncbi.nlm.nih.gov/pubmed/37093716
http://dx.doi.org/10.1099/mgen.0.000994
Descripción
Sumario:Streptococcus pyogenes genotype emm1 is a successful, globally distributed epidemic clone that is regarded as inherently virulent. An emm1 sublineage, M1(UK), that produces increased levels of SpeA toxin was associated with increased scarlet fever and invasive infections in England in 2015/2016. Defined by 27 SNPs in the core genome, M1(UK) is now dominant in England. To more fully characterize M1(UK), we undertook comparative transcriptomic and proteomic analyses of M1(UK) and contemporary non-M1(UK) emm1 strains (M1(global)). Just seven genes were differentially expressed by M1(UK) compared with contemporary M1(global) strains. In addition to speA, five genes in the operon that includes glycerol dehydrogenase were upregulated in M1(UK) (gldA, mipB/talC, pflD, and phosphotransferase system IIC and IIB components), while aquaporin (glpF2) was downregulated. M1(UK) strains have a stop codon in gldA. Deletion of gldA in M1(global) abrogated glycerol dehydrogenase activity, and recapitulated upregulation of gene expression within the operon that includes gldA, consistent with a feedback effect. Phylogenetic analysis identified two intermediate emm1 sublineages in England comprising 13/27 (M1(13SNPs)) and 23/27 SNPs (M1(23SNPs)), respectively, that had failed to expand in the population. Proteomic analysis of invasive strains from the four phylogenetic emm1 groups highlighted sublineage-specific changes in carbohydrate metabolism, protein synthesis and protein processing; upregulation of SpeA was not observed in chemically defined medium. In rich broth, however, expression of SpeA was upregulated ~10-fold in both M1(23SNPs) and M1(UK) sublineages, compared with M1(13SNPs) and M1(global). We conclude that stepwise accumulation of SNPs led to the emergence of M1(UK). While increased expression of SpeA is a key indicator of M1(UK) and undoubtedly important, M1(UK) strains have outcompeted M1(23SNPs) and other emm types that produce similar or more superantigen toxin. We speculate that an accumulation of adaptive SNPs has contributed to a wider fitness advantage in M1(UK) on an inherently successful emm1 streptococcal background.

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