Peer-reviewed veterinary case report
Live-attenuated H3N8 flu vaccine developed for dogs
By Nogales, Aitor et al.·Published in Journal of virology·2017·Department of Microbiology and Immunology, United States·View original on PubMed →
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Original publication title: Temperature-Sensitive Live-Attenuated Canine Influenza Virus H3N8 Vaccine.
- Species:
- dog
Plain-English summary
A new vaccine for canine influenza, specifically the H3N8 strain, has been developed to help protect dogs from this respiratory disease. Traditional vaccines have been less effective, but this new live-attenuated vaccine (LACIV) showed better results in tests, providing strong protection after just one dose. It works by replicating at lower temperatures, which is ideal for dogs, and has been shown to be more effective than the current inactivated vaccines. This could be a promising option for preventing canine influenza in dogs.
People also search for: dog flu vaccine · canine influenza symptoms · H3N8 vaccine for dogs · dog respiratory disease treatment
Abstract
UNLABELLED: Canine influenza is a respiratory disease of dogs caused by canine influenza virus (CIV). CIV subtypes responsible for influenza in dogs include H3N8, which originated from the transfer of H3N8 equine influenza virus to dogs; and the H3N2 CIV, which is an avian-origin virus that adapted to infect dogs. Influenza infections are most effectively prevented through vaccination to reduce transmission and future infection. Currently, only inactivated influenza vaccines (IIVs) are available for the prevention of CIV in dogs. However, the efficacy of IIVs is suboptimal, and novel approaches are necessary for the prevention of disease caused by this canine respiratory pathogen. Using reverse genetics techniques, we have developed a live-attenuated CIV vaccine (LACIV) for the prevention of H3N8 CIV. The H3N8 LACIV replicates efficiently in canine cells at 33°C but is impaired at temperatures of 37 to 39°C and was attenuated compared to wild-type H3N8 CIV in vivo and ex vivo The LACIV was able to induce protection against H3N8 CIV challenge with a single intranasal inoculation in mice. Immunogenicity and protection efficacy were better than that observed with a commercial CIV H3N8 IIV but provided limited cross-reactive immunity and heterologous protection against H3N2 CIV. These results demonstrate the feasibility of implementing a LAIV approach for the prevention and control of H3N8 CIV in dogs and suggest the need for a new LAIV for the control of H3N2 CIV. IMPORTANCE: Two influenza A virus subtypes has been reported in dogs in the last 16 years: the canine influenza viruses (CIV) H3N8 and H3N2 of equine and avian origins, respectively. To date, only inactivated influenza vaccines (IIVs) are available to prevent CIV infections. Here, we report the generation of a recombinant, temperature-sensitive H3N8 CIV as a live-attenuated influenza vaccine (LAIV), which was attenuated in mice and dog tracheal, explants compared to CIV H3N8 wild type. A single dose of H3N8 LACIV showed immunogenicity and protection against a homologous challenge that was better than that conferred with an H3N8 IIV, demonstrating the feasibility of implementing a LAIV approach for the improved control of H3N8 CIV infections in dogs.
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Search related cases →Original publication on PubMed: https://pubmed.ncbi.nlm.nih.gov/27928017/