4.5 Article

Virulence Profile, Antibiotic Resistance, and Phylogenetic Relationships among Escherichia coli Strains Isolated from the Feces and Urine of Hospitalized Patients

Journal

PATHOGENS
Volume 11, Issue 12, Pages -

Publisher

MDPI
DOI: 10.3390/pathogens11121528

Keywords

Escherichia coli; gut microbiota; urinary tract infections; ExPEC; UPEC; comparative genomics; non-lactose fermenting; antimicrobial resistance

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Through studying the clonal diversity of Escherichia coli in the guts of hospitalized patients, it was found that pathogenic E. coli strains were present in over 75% of patients' guts, with some carrying resistance genes. Furthermore, multiple ExPEC clones were identified in the guts of hospitalized patients, regardless of previous antibiotic usage.
Extra-intestinal pathogenic Escherichia coli (ExPEC) may inhabit the human gut microbiota without causing disease. However, if they reach extra-intestinal sites, common cystitis to bloodstream infections may occur, putting patients at risk. To examine the human gut as a source of endogenous infections, we evaluated the E. coli clonal diversity of 18 inpatients' guts and their relationship with strains isolated from urinary tract infection (UTI) in the same hospital. Random amplified polymorphic DNA evaluated the clonal diversity, and the antimicrobial susceptibility was determined by disk diffusion. One isolate of each clone detected was sequenced, and their virulome and resistome were determined. Overall, 177 isolates were screened, among which 32 clones were identified (mean of two clones per patient), with ExPEC strains found in over 75% of the inpatients' guts. Endogenous infection was confirmed in 75% of the cases. ST10, ST59, ST69, ST131, and ST1193 clones and critical mobile drug-resistance encoding genes (bla(CTX-M-15), bla(OXA-1), bla(DHA-1), aac(6 ')-lb-cr, mcr-1.26, qnrB4, and qnrB19) were identified in the gut of inpatients. The genomic analysis highlighted the diversity of the fecal strains, colonization by lactose-negative E. coli, the high frequency of ExPEC in the gut of inpatients without infections, and the presence of beta-lactamase producing E. coli in the gut of inpatients regardless of the previous antibiotics' usage. Considering that we found more than one ExPEC clone in the gut of several inpatients, surveillance of inpatients' fecal pathogens may prevent UTI caused by E. coli in the hospital and dissemination of risk clones.

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