Emerging Microbes and Infections (Jan 2021)

Prime-boost vaccination of mice and rhesus macaques with two novel adenovirus vectored COVID-19 vaccine candidates

  • Shengxue Luo,
  • Panli Zhang,
  • Bochao Liu,
  • Chan Yang,
  • Chaolan Liang,
  • Qi Wang,
  • Ling Zhang,
  • Xi Tang,
  • Jinfeng Li,
  • Shuiping Hou,
  • Jinfeng Zeng,
  • Yongshui Fu,
  • Jean-Pierre Allain,
  • Tingting Li,
  • Yuming Zhang,
  • Chengyao Li

DOI
https://doi.org/10.1080/22221751.2021.1931466
Journal volume & issue
Vol. 10, no. 1
pp. 1002 – 1015

Abstract

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COVID-19 vaccines are being developed urgently worldwide. Here, we constructed two adenovirus vectored COVID-19 vaccine candidates of Sad23L-nCoV-S and Ad49L-nCoV-S carrying the full-length gene of SARS-CoV-2 spike protein. The immunogenicity of two vaccines was individually evaluated in mice. Specific immune responses were observed by priming in a dose-dependent manner, and stronger responses were obtained by boosting. Furthermore, five rhesus macaques were primed with 5 × 109 PFU Sad23L-nCoV-S, followed by boosting with 5 × 109 PFU Ad49L-nCoV-S at 4-week interval. Both mice and macaques well tolerated the vaccine inoculations without detectable clinical or pathologic changes. In macaques, prime-boost regimen induced high titers of 103.16 anti-S, 102.75 anti-RBD binding antibody and 102.38 pseudovirus neutralizing antibody (pNAb) at 2 months, while pNAb decreased gradually to 101.45 at 7 months post-priming. Robust T-cell response of IFN-γ (712.6 SFCs/106 cells), IL-2 (334 SFCs/106 cells) and intracellular IFN-γ in CD4+/CD8+ T cell (0.39%/0.55%) to S peptides were detected in vaccinated macaques. It was concluded that prime-boost immunization with Sad23L-nCoV-S and Ad49L-nCoV-S can safely elicit strong immunity in animals in preparation of clinical phase 1/2 trials.

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