In vivo animal models confirm an increased virulence potential and pathogenicity of the NAP1/RT027/ST01 genotype within the Clostridium difficile MLST Clade 2

Josué Orozco-Aguilar; Alejandro Alfaro-Alarcón; Luis Acuña-Amador; Esteban Chaves-Olarte; César Rodríguez; Carlos Quesada-Gómez

doi:10.1186/s13099-020-00383-4

Gut Pathogens (Sep 2020)

In vivo animal models confirm an increased virulence potential and pathogenicity of the NAP1/RT027/ST01 genotype within the Clostridium difficile MLST Clade 2

Josué Orozco-Aguilar,
Alejandro Alfaro-Alarcón,
Luis Acuña-Amador,
Esteban Chaves-Olarte,
César Rodríguez,
Carlos Quesada-Gómez

Affiliations

Josué Orozco-Aguilar: Laboratorio de Ensayos Biológicos (LEBi), Universidad de Costa Rica
Alejandro Alfaro-Alarcón: Departamento de Patología, Escuela de Medicina Veterinaria, Universidad Nacional
Luis Acuña-Amador: Centro de Investigación en Enfermedades Tropicales and Facultad de Microbiología, Universidad de Costa Rica
Esteban Chaves-Olarte: Programa de Posgrado en Microbiología, Parasitología, Química Clínica e Inmunología, Universidad de Costa Rica
César Rodríguez: Programa de Posgrado en Microbiología, Parasitología, Química Clínica e Inmunología, Universidad de Costa Rica
Carlos Quesada-Gómez: Laboratorio de Ensayos Biológicos (LEBi), Universidad de Costa Rica

DOI: https://doi.org/10.1186/s13099-020-00383-4
Journal volume & issue: Vol. 12, no. 1
pp. 1 – 10

Abstract

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Abstract Background Based on MLST analyses the global population of C. difficile is distributed in eight clades, of which Clade 2 includes the “hypervirulent” NAP1/RT027/ST01 strain along with various unexplored sequence types (STs). Methods To clarify whether this clinically relevant phenotype is a widespread feature of C. difficile Clade 2, we used the murine ileal loop model to compare the in vivo pro-inflammatory (TNF-α, IL-1β, IL-6) and oxidative stress activities (MPO) of five Clade 2 clinical C. difficile isolates from sequence types (STs) 01, 41, 67, and 252. Besides, we infected Golden Syrian hamsters with spores from these strains to determine their lethality, and obtain a histological evaluation of tissue damage, WBC counts, and serum injury biomarkers (LDH, ALT, AST, albumin, BUN, creatinine, Na+, and Cl−). Genomic distances were calculated using Mash and FastANI to explore whether the responses were dictated by phylogeny. Results The ST01 isolate tested ranked first in all assays, as it induced the highest overall levels of pro-inflammatory cytokines, MPO activity, epithelial damage, biochemical markers, and mortality measured in both animal models. Statistically indistinguishable or rather similar outputs were obtained for a ST67 isolate in tests such as tissue damage, neutrophils count, and lethal activity. The results recorded for the two ST41 isolates tested were of intermediate magnitude and the ST252 isolate displayed the lowest pathogenic potential in all animal experiments. This ordering matched the genomic distance of the ST01 isolate to the non-ST01 isolates. Conclusions Despite their close phylogenic relatedness, our results demonstrate differences in pathogenicity and virulence levels in Clade 2 C. difficile strains, confirm the high severity of infections caused by the NAP1/RT027/ST01 strain, and highlight the importance of C. difficile typing.

Published in Gut Pathogens

ISSN: 1757-4749 (Online)
Publisher: BMC
Country of publisher: United Kingdom
LCC subjects: Medicine: Internal medicine: Specialties of internal medicine: Diseases of the digestive system. Gastroenterology
Website: https://gutpathogens.biomedcentral.com/

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