Virology Journal (Aug 2020)

AIV polyantigen epitope expressed by recombinant baculovirus induces a systemic immune response in chicken and mouse models

  • Lei Yu,
  • Jun Pan,
  • Guangli Cao,
  • Mengsheng Jiang,
  • Yunshan Zhang,
  • Min Zhu,
  • Zi Liang,
  • Xing Zhang,
  • Xiaolong Hu,
  • Renyu Xue,
  • Chengliang Gong

DOI
https://doi.org/10.1186/s12985-020-01388-w
Journal volume & issue
Vol. 17, no. 1
pp. 1 – 13

Abstract

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Abstract Background The protective efficacy of avian influenza virus (AIV) vaccines is unsatisfactory due to the presence of various serotypes generated by genetic reassortment. Thus, immunization with a polyantigen chimeric epitope vaccine may be an effective strategy for protecting poultry from infection with different AIV subtypes. Methods Baculovirus has recently emerged as a novel and attractive gene delivery vehicle for animal cells. In the present study, a recombinant baculovirus BmNPV-CMV/THB-P10/CTLT containing a fused codon-optimized sequence (CTLT) of T lymphocyte epitopes from H1HA, H9HA, and H7HA AIV subtypes, and another fused codon-optimized sequence (THB) of Th and B cell epitopes from H1HA, H9HA, and H7HA AIV subtypes, driven by a baculovirus P10 promoter and cytomegalovirus CMV promoter, respectively, was constructed. Results Western blotting and cellular immunofluorescence demonstrated that the CTLT (THB) can be expressed in rBac-CMV/THB-P10/CTLT-infected silkworm cells (mammalian HEK293T cells). Furthermore, the recombinant virus, rBac-CMV-THB-CTLT, was used to immunize both chickens and mice. Conclusions The results of an indirect ELISA, immunohistochemistry, and T lymphocyte proliferation assay indicated that specific humoral and cellular responses were detected in both chicken and mice. These results suggest that rBac-CMV/THB-P10/CTLT can be developed as a potential vaccine against different AIV subtypes.

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