The EBOLAVAC consortium achieved the following results:
1.Ph1/2 randomised-controlled study, Lausanne, Switzerland: Completion of a trial to assess safety, reactogenicity and immunogenicity of a single injection of ChAd3-EBO-Z when administered to healthy volunteers at 2 different doses. Between 24/10/14 and 22/06/15, 120 subjects were randomly assigned of whom 18 were potentially to be deployed to EBOV transmission areas and 102 were not to deploy, to receive high dose vaccine (n=49), low dose vaccine (n=51) or placebo (n=20). Phase 1 results showed that vaccine has an acceptable safety profile and is immunogenic (De Santis et al., 2016. Lancet Infect Dis.). The trial is registered on ClinicalTrials.gov Identifier: NCT02289027.
2.Ph2 expanded safety and immunogenicity studies in Africa: a. Completion of a multi-centre study in 4 African countries: Cameroon (2 centres), Mali (1 centre), Nigeria (1 centre) and Senegal (2 centres) to assess safety and immunogenicity of a single i.m dose of ChAd3-EBOV in adults 18 years of age and older- N of subjects vaccinated:3013 (1508 in the ChAd3-EBOV group- 1505 in the Placebo/ChAd3-EBO-Z group). The vaccine was generally well tolerated and immunogenic in adult subjects, the trial is registered on ClinicalTrials.gov Identifier: NCT02485301, results have been posted for the Nigeria site on
http://nctr.nhrec.net/search.php?search=ebola&submit=Search(s’ouvre dans une nouvelle fenêtre); b. Completion of a multi-centre study in 2 African countries: Mali (1 centre) and Senegal (1 centre) to assess safety and immunogenicity of a single i.m dose of ChAd3-EBOV in children 1-17 years of age -N of subjects vaccinated:600 (300 in the ChAd3-EBOV/MENACWY-TT group-300 in the MENACWY-TT/ChAd3-EBOV group). The vaccine was generally well tolerated and immunogenic in children. The trial is registered on ClinicalTrials.gov Identifier: NCT02548078.
3.Booster study with MVA-GSK-EBOV: Completion of a Ph1 study in Dakar, Senegal to assess safety and immunogenicity of heterologous prime-boost immunization with ChAd3-EBOV and MVA-GSK-EBOV received 7days after prime injection in healthy Senegalese adults (18-50 years). N of subjects vaccinated:40 (20 receiving prime and boost vaccination in the same arm, 20 in the opposite arm). ChAd3-EBO Z and MVA-EBO Z were well tolerated in Senegalese adults.EBO Z GP priming followed by MVA boosting was immunogenic
The trial is registered on ClinicalTrials.gov Identifier: NCT02485912. The manuscript is in preparation and is expected to be submitted for publication in July 2018.
4.MVA-GSK-EBOV Advanced Cell Line Process Development: Process development completed by Emergent Biosolutions (activity partially funded by Wellcome Trust). Completion of GMP manufacture at 200L scale (drug substance for~25000 doses). Half of this was filled into 2500 multi-dose vials (5 doses/vial). A similar quantity remains in storage unfilled.
5.Communication dissemination and exploitation: Several communication and dissemination materials, incl.press-releases articles in press and TV/radio programs were produced and distributed;Publication of a major scientific manuscript (www.sciencedirect.com/science/article/pii/S1473309915004867); Confidential sharing of project results with governments and NGOs incl. WHO towards improved efforts to better prepare for recurring public health emergencies; Presentation at international congresses, meetings and workshops; Project website