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Bài báo - Tạp chí
16 (2024) Trang: 1120
Tạp chí: Viruses

Chimeric marker vaccine candidates, vGPE/PAPeV Erns and vGPE/PhoPeV Erns, have been generated and their efficacy and capability to differentiate infected from vaccinated animals were confirmed in previous studies. The safety profile of the two chimeric marker vaccine candidates, particularly in the potential reversion to virulence, was evaluated. Each virus was administered to pigs with a dose equivalent to the vaccination dose, and pooled tonsil homogenates were subsequently inoculated into further pigs. Chimeric virus vGPE/PAPeV Erns displayed the most substantial attenuation, achieving this within only two passages, whereas vGPE/PhoPeV Erns was detectable until the third passage and disappeared entirely by the fourth passage. The vGPE strain, assessed alongside, consistently exhibited stable virus recovery across each passage without any signs of increased virulence in pigs. In vitro assays revealed that the type I interferon-inducing capacity of vGPE/PAPeV Erns was significantly higher than that of vGPE/PhoPeV Erns and vGPE. In conclusion, the safety profile of the two chimeric marker vaccine candidates was affirmed. Further research is essential to ensure the stability of their attenuation and safety in diverse pig populations.

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