Long-term cellular immunity of vaccines for Zaire Ebola Virus Diseases.

Aurélie Wiedemann ORCID logo ; Edouard Lhomme ORCID logo ; Mélanie Huchon ; Emile Foucat ; Marion Bérerd-Camara ; Lydia Guillaumat ; Marcel Yaradouno ; Jacqueline Tambalou ; Cécile Rodrigues ; Alexandre Ribeiro ; +6 more... Abdoul Habib Béavogui ; Christine Lacabaratz ORCID logo ; Rodolphe Thiébaut ORCID logo ; Laura Richert ; Yves Lévy ORCID logo ; Prevac study team ; (2024) Long-term cellular immunity of vaccines for Zaire Ebola Virus Diseases. Nature communications, 15 (1). 7666-. ISSN 2041-1723 DOI: 10.1038/s41467-024-51453-z
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Recent Ebola outbreaks underscore the importance of continuous prevention and disease control efforts. Authorized vaccines include Merck's Ervebo (rVSV-ZEBOV) and Johnson & Johnson's two-dose combination (Ad26.ZEBOV/MVA-BN-Filo). Here, in a five-year follow-up of the PREVAC randomized trial (NCT02876328), we report the results of the immunology ancillary study of the trial. The primary endpoint is to evaluate long-term memory T-cell responses induced by three vaccine regimens: Ad26-MVA, rVSV, and rVSV-booster. Polyfunctional EBOV-specific CD4+ T-cell responses increase after Ad26 priming and are further boosted by MVA, whereas minimal responses are observed in the rVSV groups, declining after one year. In-vitro expansion for eight days show sustained EBOV-specific T-cell responses for up to 60 months post-prime vaccination with both Ad26-MVA and rVSV, with no decline. Cytokine production analysis identify shared biomarkers between the Ad26-MVA and rVSV groups. In secondary endpoint, we observed an elevation of pro-inflammatory cytokines at Day 7 in the rVSV group. Finally, we establish a correlation between EBOV-specific T-cell responses and anti-EBOV IgG responses. Our findings can guide booster vaccination recommendations and help identify populations likely to benefit from revaccination.


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