Complete Protection of Nasal and Lung Airways Against SARS-CoV-2 Challenge by Antibody Plus Th1 Dominant N- and S-Specific T-Cell Responses to Subcutaneous Prime and Thermally-Stable Oral Boost Bivalent hAd5 Vaccination in an NHP Study

  1. Elizabeth Gabitzsch
  2. Jeffrey T. Safrit
  3. Mohit Verma
  4. Adrian Rice
  5. Peter Sieling
  6. Lise Zakin
  7. Annie Shin
  8. Brett Morimoto
  9. Helty Adisetiyo
  10. Raymond Wong
  11. Ashish Bezawada
  12. Kyle Dinkins
  13. Joseph Balint
  14. Victor Peykov
  15. Hermes Garban
  16. Philip Liu
  17. Pete Bone
  18. Andrew Bacon
  19. Jeff Drew
  20. Daniel C. Sanford
  21. Patricia Spilman
  22. Lennie Sender
  23. Shahrooz Rabizadeh
  24. Kayvan Niazi
  25. Patrick Soon-Shiong
1 evaluations Published on
Read the full article Related papers
This article on Sciety

Abstract

We have developed a dual-antigen COVID-19 vaccine incorporating genes for a modified SARS-CoV-2 spike (S-Fusion) protein and the viral nucleocapsid (N) protein with an Enhanced T-cell Stimulation Domain (N-ETSD) with the potential to increase MHC class I/II responses. The adenovirus serotype 5 platform used, hAd5 [E1-, E2b-, E3-], previously demonstrated to be effective in the presence of Ad immunity, can be delivered in an oral formulation that overcomes cold-chain limitations. The hAd5 S-Fusion + N-ETSD vaccine was evaluated in rhesus macaques showing that a subcutaneous prime followed by oral boosts elicited both humoral and Th1 dominant T-cell responses to both S and N that protected the upper and lower respiratory tracts from high titer (1 x 10 6 TCID 50 ) SARS-CoV-2 challenge. Notably, viral replication was inhibited within 24 hours of challenge in both lung and nasal passages, becoming undetectable within 7 days post-challenge.

ONE SENTENCE SUMMARY

hAd5 spike + nucleocapsid SC prime/oral boost vaccine elicits humoral and T-cell responses and protects rhesus macaques from SARS-CoV-2 challenge.

Related articles

Related articles are currently not available for this article.