Phase II/III Double-Blind Study Evaluating Safety and Immunogenicity of a Single Intramuscular Booster Dose of the Recombinant SARS-CoV-2 Vaccine “Patria” (AVX/COVID-12) Using an Active Newcastle Disease Viral Vector (NDV) during the Omicron Outbreak in Healthy Adults with Elevated Baseline Antibody Titers from Prior COVID-19 and/or SARS-CoV-2 Vaccination

  1. Constantino López-Macías
  2. Martha Torres
  3. Brenda Armenta-Copca
  4. Niels H. Wacher
  5. Arturo Galindo-Fraga
  6. Laura Castro-Castrezana
  7. Andrea Alicia Colli-Domínguez
  8. Edgar Cervantes-Trujano
  9. Isabel Erika Rucker-Joerg
  10. Fernando Lozano-Patiño
  11. Juan José Rivera-Alcocer
  12. Abraham Simón-Campos
  13. Efrén Alberto Sánchez-Campos
  14. Rafael Aguirre-Rivero
  15. Alejandro José Muñiz-Carvajal
  16. Luis del Carpio-Orantes
  17. Francisco Márquez-Díaz
  18. Tania Rivera-Hernández
  19. Alejandro Torres-Flores
  20. Luis Ramírez-Martínez
  21. Georgina Paz-De la Rosa
  22. Oscar Rojas-Martínez
  23. Alejandro Suárez-Martínez
  24. Gustavo Peralta-Sánchez
  25. Claudia Carranza
  26. Esmeralda Juárez
  27. Horacio Zamudio-Meza
  28. Laura E. Carreto-Binaghi
  29. Mercedes Viettri
  30. Damaris Romero-Rodríguez
  31. Andrea Palencia
  32. David Sarfati-Mizrahi
  33. Weina Sun
  34. Héctor Elías Chagoya-Cortés
  35. Felipa Castro-Peralta
  36. Peter Palese
  37. Florian Krammer
  38. Adolfo García-Sastre
  39. Bernardo Lozano-Dubernard
Read the full article See related articles

Listed in

This article is not in any list yet, why not save it to one of your lists.
Log in to save this article

Abstract

Background

The urgent need for safe, effective, and economical coronavirus disease 2019 (COVID-19) vaccines, especially for booster campaigns targeting vulnerable populations, prompted the development of the AVX/COVID-12 vaccine candidate. AVX/COVD-12 is based in a Newcastle disease virus La Sota (NDV-LaSota) recombinant viral vector. This vaccine expresses a stabilized version of the spike protein of severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), specifically the ancestral Wuhan strain. The study aimed to assess its safety, immunogenicity, and potential efficacy as an anti-COVID-19 booster vaccine.

Methods

In a phase II/III clinical trial conducted from November 9, 2022, to September 11, 2023, a total of 4,056 volunteers were enrolled. Participants received an intramuscular booster dose of either AVX/COVID-12 or AZ/ChAdOx-1-S vaccines. Safety, immunogenicity, and potential efficacy were assessed through various measures, including neutralizing antibody titers, interferon (IFN)-γ-producing CD4+ T cells, and CD8+ T cells. The evaluation also involved immunobridging, utilizing the AZ/ChAdOx-1-S vaccine as an active comparator, and monitoring the incidence of COVID-19 cases.

Findings

The AVX/COVID-12 vaccine induced neutralizing antibodies against both the ancestral SARS-CoV-2 and the BA.2 and BA.5 Omicron variants. The geometric mean ratio of neutralizing antibody titers between individuals immunized with the AVX/COVID-12 vaccine and those with the AZ/ChAdOx-1-S vaccine at 14 days is 0.96, with a confidence interval (CI) of 0.85-1.06. The outcome aligns with the non-inferiority criterion recommended by the World Health Organization (WHO), indicating a lower limit of the CI greater than or equal to 0.67. Induction of IFN-γ-producing CD8+ T cells at day 14 post-immunization was exclusively observed in the AVX/COVID-12 group. Finally, a trend suggested a potentially lower incidence of COVID-19 cases in AVX/COVID-12 boosted volunteers compared to AZ/ChAdOx-1-S recipients.

Conclusion

The AVX/COVID-12 vaccine proved safe, well-tolerated, and immunogenic. AVX/COVID-12 meets the WHO non-inferiority standard compared to AZ/ChAdOx-1-S. These results strongly advocate for AVX/COVID-12 as a viable booster dose, supporting its utilization in the population.

Article activity feed

  1. Version published to 10.1101/2024.02.11.24302530v1 on medRxiv