# Molecular epidemiology and antimicrobial resistance in Clostridioides difficile strains isolated from children and adolescents in a tertiary referral pediatric hospital in Fortaleza, Brazil

**Authors:** Hildenia Baltasar Ribeiro Nogueira, Cecília Leite Costa, Carlos Quesada-Gómez, Dvison de Melo Pacífico, Eliane de Oliveira Ferreira, Renata Ferreira de Carvalho Leitão, Gerly Anne de Castro Brito

PMC · DOI: 10.1016/j.bjid.2024.103767 · The Brazilian Journal of Infectious Diseases · 2024-06-03

## TL;DR

This study examines Clostridioides difficile infections in children in northeastern Brazil, finding a high frequency of infection and identifying new strains.

## Contribution

The study reports the first molecular epidemiology and antimicrobial resistance data of C. difficile in children from northeastern Brazil.

## Key findings

- C. difficile was isolated from 35% of samples, with 30.4% of samples showing toxin positivity.
- Four toxigenic strains were identified, including new PCR ribotypes and PFGE-pulsotypes.
- All toxigenic strains were sensitive to metronidazole and vancomycin, and chronic diseases were main risk factors.

## Abstract

C. difficile has been increasingly reported as a cause of gastrointestinal disease in children, ranging from mild self-limiting diarrhea to severe conditions such as pseudomembranous colitis and toxic megacolon. Only two pediatric research groups reported the presence of C. difficile infection in Brazilian children, but no previous research has examined C. difficile infection among children in northeastern Brazil. This prospective cross-sectional study investigated the molecular epidemiology and antimicrobial resistance of C. difficile strains isolated from children and adolescents with diarrhea referred to a tertiary pediatric hospital in Brazil while exploring the associated risk factors.

Toxin positivity or C. difficile isolation was found in 30.4 % (17/56) samples. C. difficile was isolated from 35 % (6/17) samples. Four toxigenic strains were identified (tpi+, tcdA+, tcdB+, cdtB-, without tcdC deletions) belonging to PCR ribotypes and PFGE-pulsotypes: 046 (new pulsotype 1174), 106 (NAP11), 002 (new pulsotype 1274), 012 (new pulsotype NML-1235). Two of the six isolates belonging to ribotypes 143 and 133 were non-toxigenic. All toxigenic strains were sensitive to metronidazole and vancomycin. Regarding the clinical manifestation, diarrhea lasted an average of 11 days, ranging from 3 to 50 days and was often associated with mucus and/or blood. All six patients from whom the C. difficile was isolated had a chronic disease diagnosis, with these comorbidities as the main risk factors.

Our study enhances our understanding of the present epidemiological landscape of C. difficile-associated diarrhea (CDI) among children in northeastern Brazil, reveling a substantial CDI frequency of 30.4 %, with toxigenic strains detected in 76.4 % of cases, highlighting a higher prevalence compared to earlier Brazilian studies. In the globalized world, an understanding of disease-generating strains, the associated risk factors, clinical manifestation, and antimicrobial sensitivity has fundamental epidemiological importance and draws attention to preventive measures, allowing for more decisive action.

## Linked entities

- **Chemicals:** metronidazole (PubChem CID 4173), vancomycin (PubChem CID 14969)
- **Diseases:** diarrhea (MONDO:0001673), pseudomembranous colitis (MONDO:0000705), toxic megacolon (MONDO:0002105)
- **Species:** Clostridioides difficile (taxon 1496)

## Full-text entities

- **Genes:** cdtB [NCBI Gene 982], TPI1 (triosephosphate isomerase 1) [NCBI Gene 7167] {aka HEL-S-49, TIM, TPI, TPID}
- **Diseases:** pseudomembranous colitis (MESH:D004761), toxic megacolon (MESH:D008532), C. difficile-associated diarrhea (MESH:D003967), gastrointestinal disease (MESH:D005767), C. difficile infection (MESH:D003015)
- **Species:** Homo sapiens (human, species) [taxon 9606], Clostridioides difficile (species) [taxon 1496]

## Full text

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## Figures

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## References

29 references — full list in the complete paper: https://tomesphere.com/paper/PMC11215949/full.md

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Source: https://tomesphere.com/paper/PMC11215949