4.6 Article

Blocking Interhost Transmission of Influenza Virus by Vaccination in the Guinea Pig Model

Journal

JOURNAL OF VIROLOGY
Volume 83, Issue 7, Pages 2803-2818

Publisher

AMER SOC MICROBIOLOGY
DOI: 10.1128/JVI.02424-08

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Funding

  1. NIAID [HHSN 266200700010C]
  2. W.M. Keck Foundation
  3. Center for Investigating Viral Immunity and Antagonism [1 UC19 AI062623-023]
  4. Sunnybrook Health Sciences Centre, Toronto, Canada
  5. Ruth L. Kirschstein Physician Scientist Research Training in Pathogenesis of Viral Diseases award [ST32A1007623-07]

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Interventions aimed at preventing viral spread have the potential to effectively control influenza virus in all age groups, thereby reducing the burden of influenza illness. For this reason, we have examined the efficacy of vaccination in blocking the transmission of influenza viruses between guinea pigs. Three modes of immunization were compared: (i) natural infection; (ii) intramuscular administration of whole, inactivated influenza virus in 2 doses; and (iii) intranasal inoculation with live attenuated influenza virus in 2 doses. The ability of each immunization method to block the spread of a homologous (A/Panama/2007/99) H3N2 subtype and a heterologous (A/Wisconsin/67/05) H3N2 subtype influenza virus was tested. We found that previous infection through a natural route provided sterilizing immunity against both homologous and heterologous challenges; thus, no transmission to or from previously infected animals was observed. Vaccination with an inactivated influenza virus vaccine, in contrast, did not prevent guinea pigs from becoming infected upon challenge with either virus. Thus, both intranasal inoculation and exposure to an acutely infected guinea pig led to the infection of vaccinated animals. Vaccination with inactivated virus did, however, reduce viral load upon challenge and decrease the number of secondary transmission events from vaccinated animals to naive cage mates. Vaccination with a live attenuated virus was found to be more efficacious than vaccination with inactivated virus, resulting in sterilizing immunity against homologous challenge and full protection against the transmission of the homologous and heterologous viruses to naive contacts. In conclusion, we have shown that the guinea pig model can be used to test influenza virus vaccines and that the efficiency of transmission is a valuable readout when vaccine efficacy is evaluated.

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