On December 2nd, 2022, the Health Security Agency from London (United Kingdom, UK) alerted of an increase of Streptococcus pyogenes (Group A Streptococcus, GAS) invasive infections.1 Characterization of the GAS isolates showed that the recently described M1UK clone and emm12 were predominant during the outbreak. The emergence of the S. pyogenes clone during the UK alert period has raised concerns about the potential spread and impact of these strains,2 especially when the M1UK clone has been reported in other countries.2,3

In the pre COVID-19 pandemic period, the National Center for Microbiology of Spain (National Institute Carlos III) reported the first nationwide microbiological, epidemiological and characterization study of invasive GAS disease between 2007 and 2019 being the emm1, emm89, and emm3 the most prevalent emm types in our country.4

Meanwhile, in Madrid (Spain), it has been recently reported an increase of the GAS infections in children compared with the first two pandemic COVID-19 years (2020–2021)5 and a non-significant increase of S. pyogenes bloodstream infections (GAS-BSI) in children population.6

The aim of this study was to investigate possible changes on the genomic epidemiology and incidence of invasive GAS at our tertiary care center, focusing on bloodstream infections, during the UK alert period (2023).

We recovered all GAS isolated from blood cultures between January and May 2023. Blood cultures were incubated using the Virtuo™ system (BioMérieux®, Marcy l’Etoile, France) and identified according to the protocol described by García-Clemente et al.7

Demographic, clinical, and analytical data of patients with GAS-BSI was retrospectively collected from the hospital medical records.

S. pyogenes DNA extraction was carried out using the DNeasy® blood & Tissue kit (Qiagen GmbH, Hilden, Germany) and sequenced in the Ion GeneStudio S5 system (Thermo Fisher Scientific, Massachusetts, EEUU) using the NEBNext® Fast DNA Library Prep Set for Ion Torrent™ (New England Biolabs, Ipswich MA, USA). Genome assembly was performed using spades v3.14.1 (https://github.com/ablab/spades) and emm typing using the emmtyper tool v0.2.0 (https://github.com/MDU-PHL/emmtyper)

Analysis of virulence genes was performed using abricate v1.0.1 (https://github.com/tseemann/abricate) and the Virulence Factor DataBase (https://www2.cdc.gov/vaccines/biotech/strepblast.asp). Determination of the M1UK/global clone analysis through SNP analysis using the Geneious prime 2023.0.2.8 software. Sequencing data of all isolates are available at the European Nucleotide Archive (ENA) under the Project PRJEB64433.

Antimicrobial susceptibility was performed using the microdilution method with MicroScan Walkaway™ (Beckman Coulter®, Indianapolis, IN, USA) system using the MSTRP+ 6 panel. The MIC values were interpreted following EUCAST breakpoints, version 12.0 (http://www.eucast.org/clinical_breakpoints/).

We diagnosed 35 cases of GAS-BSI during the months of January–May of the years 2017–2023. Between 2017 and 2022, there were 21 cases with a median number of 3.5 [IQR=2.5–4.5] per year, while the number of cases during the same period in 2023 reached 14 (Table 1). During the 2017–2022 period, there were 9 out of 21 GAS-BSI cases in pediatric population (42.9%) with a mean age of 4 years while in the 2023 period and only 3 out of 14 cases occurred in children (21.43%) with a mean age of 7 years. In relation to the focus of GAS-BSI bloodstream infections in 2023, ten out of the 14 patients (71.4%) had a cutaneous focus, three of 14 (21.4%) had a respiratory portal of entry and one patient (7.2%) had an abdominal focus. Twelve of the 14 patients (85.71%) were pregnant women or had a previous pathology such as transplantation, diabetes, COPD or cancer.

According to the WGS analysis of 2023 GAS-BSI isolates, we reported eight emm types: emm1, emm12, emm4, emm5, emm11, emm22, emm28, and emm109 being the most frequent the emm1 (6/14, 42.9%), and emm12 (2/14, 14.3%) (Fig. 1). Among the six GAS emm1, five out of the six emm1 types (83.3%) presented the 27 SNPs associated with the M1UK clone. The fourteen GAS-BSI isolates were susceptible to beta-lactams, macrolides, clindamycin and fluoroquinolones.

Fig. 1.

emm types and superantigen genes of S. pyogenes bacteremia during January–May 2023. The figure shows the presence (green) or absence (gray) of virulence genes among the S. pyogenes emm types. The ENA accession to the isolate reads is located on the right column.

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We analyzed the presence of 11 superantigen genes for each GAS-BSI isolated sequenced by WGS including smeZ, speA, speC, speG, speH, speI, speJ, speK, speL, speM and ssa genes. The mainly superantigen genes found were the streptococcal mitogenic exotoxin Z (smeZ) (14/14, 100%), followed by speG (12/14, 85.7%), speC (10/14, 71.4%), and speJ (7/14, 50%) genes. All five emm1 M1UK clones had speA and speJ superantigen genes. However, the only M1global clone had speJ but not speA superantigen genes.

The emergence of the M1UK clone and emm12 strains in the United Kingdom raised concerns about their potential spread and impact, especially when such increase of cases has been also reported in other countries such as France, the Netherlands, Finland, Sweden or USA.9–12

In the same way, our findings indicate an increase in the number of GAS-BSI in our setting during January–May 2023 compared to the same period in previous years but, contrary to other countries reports, at the expense of the increase in the number of cases in adults. As there have been no changes in the attended population or blood culture extraction protocols in children, the cause of this discrepancy is yet unknown and will be studied in the future. However, it is important to highlight that in the two years prior to the increase in GAS-BSI cases, marked by the SARS-CoV-2 pandemic, the number of cases were exceptionally low, so it is plausible a relationship between the two events. In addition, our current genomic epidemiology of GAS-BSI seems dominated by the M1UK clone followed by the emm12, similar to the data reported in the UK during the GAS alert 2022–2023. This should bring the attention as the M1UK clone detected in Madrid produces both the speA and speJ superantigens that might be related to higher invasiveness of these strains.13,14

Our main limitation is that we have not characterized the S. pyogenes strains isolated from blood cultures in our setting in the 2017–2022 period. Nonetheless, this limitation is compensated by the extensive national and local data published in previous years.4 Moreover, we did not include in our study other invasive GAS samples (pleural fluid, CSF, pneumonia, necrotizing fasciitis) as they were scarce and more heterogeneous.

In conclusion, this study provides preliminary insights into the genomic epidemiology and incidence of GAS-BSI during the UK alert period in 2023. The observed increase in GAS-BSI cases overall, but not in children, suggests differences in the affected population in our environment. The predominance of the M1UK clone and the presence of specific superantigen genes among the isolates highlight the need for continued surveillance and further investigation into the molecular characteristics and clinical implications of circulating GAS strains.

Ethical review and approval were not required for the study on human participants in accordance with the local legislation and institutional requirements. The data used are from clinical samples that were necessary for the clinical diagnosis of the patients. The epidemiological S. pyogenes study was not included in the clinical report of the patients.

Not funding.

None declared.