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Peer-reviewed veterinary case report

How well parvovirus vaccines work in puppies with maternal antibodies

By Pearce, Jacqueline et al.·Published in Vaccines·2025·MSD Animal Health, 5831 Boxmeer, The Netherlands, Netherlands·View original on Crossref

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Original publication title: Assessing Canine Parvovirus Vaccine Performance in Puppies with Maternally Derived Antibody: An Improved Study Design

Species:
dog

Plain-English summary

A group of 6-week-old puppies was tested to see how well different canine parvovirus vaccines worked, especially in those with antibodies passed from their mothers. The puppies were paired, with one vaccinated and the other left unvaccinated as a control. The puppies vaccinated with the Nobivac DP PLUS vaccine showed the best results, developing strong immunity and shedding the vaccine virus, which helped the unvaccinated pups also develop immunity. This study highlights that not all vaccines are equally effective in puppies with maternal antibodies, and the Nobivac DP PLUS vaccine performed the best in this case.

People also search for: puppy parvovirus vaccine effectiveness · canine parvovirus vaccine for puppies · Nobivac DP PLUS vaccine review

Abstract

Background/Objectives: Typically, studies aiming to assess the ability of canine parvovirus (CPV) vaccines to immunise puppies with maternally derived antibody (MDA) are undertaken using group-housed puppies. Since live attenuated vaccine virus is invariably shed in the faeces, this can result in repeated oral re-exposure and puppies which failed to respond to the initial vaccination may respond instead to shed vaccine virus in the environment, thus artificially enhancing the efficacy of the vaccine. This problem can be avoided by adopting a pair-housed study design where one vaccinated pup is housed with one unvaccinated sentinel. Using this design, we examine the capability of four commercially available canine parvovirus vaccines to immunise MDA-positive pups. Methods: Thirty-four 6-week-old puppies born to vaccinated dams were divided into four vaccine groups with similar MDA ranges. Within each group puppies were paired based on matching MDA titres, and each pair was housed in separate biocontainment accommodation. In each pair, the pup with the highest MDA was vaccinated and the other left as an unvaccinated sentinel. All vaccinates were given a single dose of one of the vaccines. Vaccinates and sentinels were then bled every 2–4 days and CPV antibody was measured. Daily rectal swabs were also collected from all pups to identify any shed vaccinal CPV. Results: All the pups vaccinated with Nobivac DP PLUS seroconverted, with significantly higher antibody titres compared to the pups in other vaccine groups, all shed vaccine virus, and all bar one of the sentinel pups seroconverted. In the other groups, only vaccinated pups with lower levels of MDA seroconverted and shed vaccine virus but none of the sentinel pups seroconverted. Conclusions: Different canine parvovirus vaccines differ in their ability to replicate in and immunise puppies with MDA, the levels of which may vary widely between individuals. The shedding of vaccinal CPV is an important consideration when designing studies to demonstrate efficacy in MDA-positive puppies.

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Original publication on Crossref: https://doi.org/10.3390/vaccines13080832