Expert Review of Vaccines (Aug 2017)

Development and identification of a new Vero cell-based live attenuated influenza B vaccine by a modified classical reassortment method

  • Fan Yang,
  • Lei Ma,
  • Jian Zhou,
  • Yinjie Wu,
  • Jingxia Gao,
  • Shaohui Song,
  • Xingliang Geng,
  • Qi Guo,
  • Zhuofan Li,
  • Weidong Li,
  • Guoyang Liao,
  • Yufeng Li

DOI
https://doi.org/10.1080/14760584.2017.1337514
Journal volume & issue
Vol. 16, no. 8
pp. 855 – 863

Abstract

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Background: It was to generate a new Vero and cold-adapted live attenuated influenza B vaccine with enough safety and immunogenicity. Methods: According to modified classical reassortment method, the donor strain was B/Yunnan/2/2005Vca(B), and the parental virus strain was B/Brisbane/60/2008wt. After co-infection in Vero cells, the prepared antibody serum inhibited the donor strain growth, and screening conditions inhibited the parental virus growth, which induced the growth of the new reassortant virus B/Brisbane/60/2008Vca(B) grow. Through intraperitoneal injection (i.j.) and intranasal injection (n.j.) we evaluated the safety and immunogenicity of the vaccine. Results: A high-yield of the reassortant virus was produced in Vero cells at 25°C, similar to the donor strains. After sequencing, it was found that B/Brisbane/60/2008Vca(B) Hemagglutinin (HA) and Neuraminidase (NA) gene fragments were from B/Brisbane/60/2008wt, while the other 6 gene fragments were from B/Yunnan/2/2005Vca(B). The n.j. immune pathway experiments showed no significant differences between the treatment and the PBS control group with respect to weight changes (P > 0.5). Furthermore, the new strain had a sufficient geometric mean titter (GMT) against B/Brisbane/60/2008wt. Conclusion: The new reassortant live attenuated influenza B vaccine was safe and having enough immune stimulating ability.

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