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Escherichia coli encoding Shiga toxin subtype Stx2f causing human infections in England, 2015-2022

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JOURNAL OF MEDICAL MICROBIOLOGY
卷 72, 期 6, 页码 -

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MICROBIOLOGY SOC
DOI: 10.1099/jmm.0.001707

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Shiga toxin-producing Escherichia coli; Shiga toxin subtype; public health surveillance; haemolytic uraemic syndrome

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This study analyzed clinical outcomes and genome-sequencing data of STEC encoding-stx2f infections in England to assess the risk to public health. The results showed that STEC harboring stx2f can cause severe clinical outcomes, including STEC-HUS. Therefore, it is recommended to strengthen the collection and sharing of microbiological and epidemiological data and further study the animal and environmental reservoirs and transmission routes.
Introduction. Shiga toxin-producing Escherichia coli (STEC) belong to a diverse group of gastrointestinal pathogens defined by the presence of Shiga toxin genes (stx) of which there are at least ten subtypes (Stx1a- Stx1d and Stx2a-Stx2g). Gap Statement. Initially thought to be associated with mild symptoms, more recently STEC encoding stx2f have been iso-lated from cases of haemolytic uraemic syndrome (HUS) and the clinical significance and public health burden require further investigation. Aim. We analysed clinical outcomes and genome-sequencing data linked to patients infected with STEC encoding-stx2f in England to assess the risk to public health. Methodology. One hundred and twelve E. coli (n=58 isolates encoded stx2f; n=54 isolates E. coli belonging to CC122 or CC722 that had eae but were negative for stx) isolated from patients' faecal specimens between 2015 and 2022 were genome sequenced and linked to epidemiological and clinical outcome data. All isolates were investigated for the presence of virulence genes and a maximum-likelihood phylogeny of isolates belonging to CC122 and CC722 was constructed. Results. There were 52 cases infected with STEC harbouring stx2f between 2015 and 2022, with the majority identified in 2022. Most cases resided in the North of England (n=39/52, 75 %), were female (n=31, 59.6 %) and/or aged five and under (n=29, 55.8 %). Clinical outcome data were available for 40/52 cases (76.9 %) and 7/40(17.5 %) were diagnosed with STEC- HUS. In the two most common clonal complexes, CC122 and CC722, the presence of the stx2f- encoding prophage correlated with the pres-ence of additional virulence genes, astA, bfpA and cdt, located on an 85kbp IncFIB plasmid. Conclusions. Certain serotypes of E. coli harbouring stx2f cause severe clinical outcomes, including STEC- HUS. Public health advice and possible interventions are limited, as little is known about the animal and environmental reservoirs and transmis-sion routes. We recommend more comprehensive and standardized collection of microbiological and epidemiological data, and routine sharing of sequencing data between public health agencies worldwide.

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