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Characterization of emerging novel human astrovirus: from bedside to bench

  • Autores: Vu Diem Lan Cantero
  • Directores de la Tesis: Albert Bosch Navarro (dir. tes.), Susana Guix Arnau (codir. tes.)
  • Lectura: En la Universitat de Barcelona ( España ) en 2020
  • Idioma: inglés
  • Tribunal Calificador de la Tesis: Tomàs Pumarola Suñé (presid.), Javier Buesa Gómez (secret.), Vito Martella (voc.)
  • Programa de doctorado: Programa Oficial de Doctorado en Biotecnología
  • Materias:
  • Enlaces
    • Tesis en acceso abierto en: TESEO
  • Resumen
    • We implemented several cell culture systems for the propagation of novel human astrovirus (HAstV) MLB: HAstV-MLB1 and HAstV-MLB2 could be propagated on HuH-7 and A549 cell lines and establish persistent infection. Only a few proportion of cells were infected (5-10%), but the viral titre in the supernatant was high (7-10 log10 genome copies/ml of supernatant). Depending on the cell culture and genotype, we observed no or a delayed and reduced interferon response during acute infection and no interferon response during persistent infection. Similarly, exogenous interferon-β could cure HuH-7 from HAstV MLB1 persistent infection, but had no effect on viral replication in A549 cell lines. In our first epidemiological study, we observed a prevalence of 10% for novel HAstV in stool samples of children < 5 years old with undiagnosed gastroenteritis, with a predominance in children under 2 years old. There was a high rate of co-infection with other enteric viruses (66%), and Cq value was not different between mono- and co-infected cases. In the second epidemiological study, we did not find a difference in the prevalence of novel HAstV when comparing children with undiagnosed gastroenteritis (6.3%) and asymptomatic children (4%). Nevertheless, we found that asymptomatic children had a higher median viral titre (6.52 log10 viral RNA copy number/ml of fecal suspension IQR 4.52-6.84) than symptomatic children (2.35 log10 viral RNA copy number/ml of fecal suspension, IQR 2.13-3.76). We also found that among symptomatic children, novel HAstV viral titre was higher in coproculture-positive cases (5.19 log10 viral RNA copy number/ml of fecal suspension, IQR 4.24-6.22) than in coproculture-negative ones (2.31 log10 viral RNA copy number/ml of fecal suspension, IQR 2.11-3.32). We could not find risk factor that can predict the occurrence of novel HAstV infection.


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