Abstract

Norovirus (NoV) is a leading cause of gastroenteritis and genotype II.4 (GII.4) is responsible for the majority of nosocomial NoV infections. Our objective was to examine whether sequencing of the capsid gene might be a useful tool for the hospital outbreak investigation to define possible transmission routes. All NoV positive samples submitted from one university hospital during the 2007/8 season were selected. Genotyping of selected samples by partial polymerase gene sequencing had shown that the majority belonged to the GII.4 variant Den Haag 2006b and had identical polymerase sequences. Sequences of the capsid gene (1412 nucleotides) were obtained from the first available sample from 55 patients. From six immunocompromised patients with persistent infections a second sample was also included. As a control for a point-source outbreak, five samples from a foodborne outbreak caused by the same GII.4 variant were analyzed. Forty-seven of the inpatients (85%) were infected with the GII.4 variant Den Haag 2006b. Phylogenetic analysis of the Den Haag 2006b sequences identified four distinct outbreaks in different departments and a fifth outbreak with possible inter-department spread. In addition, a more heterogeneous cluster with evidence of repeated introductions from the community, but also possible inter-department spread was observed. In all six patients with paired sequences, evidence for in vivo evolution of the virus was found. Capsid gene sequencing showed substantial sequence variation among NoV GII.4 variant Den Haag 2006b strains from one single institution during a nine months’ period. This method proved useful to understand the local epidemiology and, when used promptly, has the potential to make infection control measures more targeted.

Highlights

  • Norovirus (NoV) is a leading cause of acute gastroenteritis worldwide, causing both outbreaks and sporadic cases [1,2,3,4,5,6]

  • The first available sample from each patient was included for analysis with a GII.4 specific reverse transcription polymerase chain reaction (RT-PCR)

  • Five samples from a foodborne outbreak caused by GII.4 variant Den Haag 2006b, occurring in 2008, were included in the study in order to analyze the capsid gene sequence variation in a known point-source outbreak

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Summary

Introduction

Norovirus (NoV) is a leading cause of acute gastroenteritis worldwide, causing both outbreaks and sporadic cases [1,2,3,4,5,6]. It is a positive-sense single-stranded non-enveloped RNA-virus belonging to the family Caliciviridae. The genotype II. (GII.4) is responsible for the majority of infections in healthcare settings [3]. Novel GII. variants emerge periodically and spread in a pandemic manner [8, 9] and there is growing evidence that this is due to antigenic drift in response to selective pressure from the host population [10,11,12,13]

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