Differentiation between Wild-Type Group A Rotaviruses and Vaccine Strains in Cases of Suspected Horizontal Transmission and Adverse Events Following Vaccination

Sonja Jacobsen; Sandra Niendorf; Roswitha Lorenz; C-Thomas Bock; Andreas Mas Marques

doi:10.3390/v14081670

Differentiation between Wild-Type Group A Rotaviruses and Vaccine Strains in Cases of Suspected Horizontal Transmission and Adverse Events Following Vaccination

Viruses. 2022 Jul 29;14(8):1670. doi: 10.3390/v14081670.

Authors

Sonja Jacobsen^{1

2}, Sandra Niendorf^{1

2}, Roswitha Lorenz^{1

2}, C-Thomas Bock^{1

3}, Andreas Mas Marques^{1

2}

Affiliations

¹ Unit Gastroenteritis and Hepatitis Viruses and Enteroviruses, Department of Infectious Diseases, Robert Koch Institute, Seestraße 10, 13353 Berlin, Germany.
² Consultant Laboratory for Rotaviruses, Robert Koch Institute, Seestraße 10, 13353 Berlin, Germany.
³ Institute of Tropical Medicine, University of Tuebingen, Wilhelmstraße 27, 72074 Tuebingen, Germany.

Abstract

Human group A rotaviruses (RVA) are important enteric pathogens, as they are a leading cause of acute gastroenteritis (AGE) in children worldwide. Since 2013, the German Standing Committee on vaccination recommended the routine rotavirus vaccination for infants in Germany. While vaccination has significantly decreased RVA cases and worldwide mortality, in some cases, infants can develop acute gastroenteritis as an adverse reaction after immunization with an attenuated live vaccine. Pediatricians, as well as clinicians and diagnostic laboratories, contacted the Consultant Laboratory for Rotaviruses and inquired whether cases of RVA-positive AGE after vaccination were associated with vaccine or with wild-type RVA strains. A testing algorithm based on distinguishing PCRs and confirmative sequencing was designed, tested, and applied. Diagnostic samples from 68 vaccinated children and six cases where horizontal transmission was suspected were investigated in this study. Using a combination of real-time PCR, fragment-length analysis of amplicons from multiplex PCRs and confirmative sequencing, vaccine-like virus was detected in 46 samples and wild-type RVA was detected in 6 samples. Three mixed infections of vaccine and wild-type RVA were detectable, no RVA genome was found in 19 samples. High viral loads (>1.0 × 107 copies/g stool) were measured in most RVA-positive samples. Furthermore, information on co-infections with other AGE pathogens in the vaccinated study population was of interest. A commercial multiplex PCR and in-house PCRs revealed three co-infections of vaccinated infants with bacteria (two samples with Clostridioides difficile and one sample with enteropathogenic E. coli) and six co-infections with norovirus in a subset of the samples. Human astrovirus was detected in one sample, with suspected horizontal transmission. The cases of suspected horizontal transmission of vaccine RVA strains could not be confirmed, as they either involved wild-type RVA or were RVA negative. This study shows that RVA-positive AGE after vaccination is not necessarily associated with the vaccine strain and provides a reliable workflow to distinguish RVA vaccine strains from wild-type strains.

Keywords: acute gastroenteritis; adverse events; co-infections; diagnostic workflow; horizontal transmission; molecular diagnostics; rotavirus A; vaccination; virus shedding.

MeSH terms

Child
Coinfection*
Escherichia coli / genetics
Feces
Gastroenteritis*
Genotype
Humans
Infant
Phylogeny
Real-Time Polymerase Chain Reaction
Rotavirus Infections* / prevention & control
Rotavirus Vaccines* / adverse effects
Rotavirus* / genetics
Vaccination / adverse effects

Substances

Rotavirus Vaccines

Grants and funding

This research received no external funding.