Neutralizing antibody-independent immunity to SARS-CoV-2 in hamsters and hACE-2 transgenic mice immunized with a RBD/Nucleocapsid fusion protein

  1. Julia T. Castro
  2. Marcílio J. Fumagalli
  3. Natalia S. Hojo-Souza
  4. Patrick Azevedo
  5. Natalia Salazar
  6. Bruna Rattis
  7. Simone G. Ramos
  8. Lídia Faustino
  9. Gregório G. Almeida
  10. Livia I. Oliveira
  11. Tomas G. Marçal
  12. Marconi Augusto
  13. Rubens Magalhães
  14. Bruno Cassaro
  15. Gabriela Burle
  16. Daniel Doro
  17. Jorge Kalil
  18. Edson Durigon
  19. Andrés Salazar
  20. Otávia Caballero
  21. Alexandre Machado
  22. João S. Silva
  23. Flávio da Fonseca
  24. Ana Paula Fernandes
  25. Santuza R. Teixeira
  26. Ricardo T. Gazzinelli
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Abstract

The nucleocapsid (N) and the receptor binding domain (RBD) of the Spike (S) proteins elicit robust antibody and T cell responses either in vaccinated or COVID-19 convalescent individuals. We generated a chimeric protein that comprises the sequences of RBD from S and N antigens (SpiN). SpiN was highly immunogenic and elicited a strong IFNγ response from T cells and high levels of antibodies to the inactivated virus, but no neutralizing antibodies. Importantly, hamsters and the human Angiotensin Convertase Enzyme-2-transgenic mice immunized with SpiN were highly resistant to challenge with the wild type SARS-CoV-2, as indicated by viral load, clinical outcome, lung inflammation and lethality. Thus, the N protein should be considered to induce T-cell-based immunity to improve SARS-CoV-2 vaccines, and eventually to circumvent the immune scape by variants.

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