Literature DB >> 28985239

Safety and immunogenicity of rVSVΔG-ZEBOV-GP Ebola vaccine in adults and children in Lambaréné, Gabon: A phase I randomised trial.

Selidji T Agnandji1,2,3, José F Fernandes1,2, Emmanuel B Bache1, Régis M Obiang Mba1, Jessica S Brosnahan1,2,3, Lumeka Kabwende1, Paul Pitzinger1,2,4, Pieter Staarink1,5, Marguerite Massinga-Loembe1, Verena Krähling3,6, Nadine Biedenkopf6, Sarah Katharina Fehling6, Thomas Strecker6, David J Clark7, Henry M Staines7, Jay W Hooper8, Peter Silvera8, Vasee Moorthy9, Marie-Paule Kieny9, Akim A Adegnika1,2,3,10, Martin P Grobusch1,2,5, Stephan Becker3,6, Michael Ramharter1,2,4, Benjamin Mordmüller1,2,3, Bertrand Lell1,2,3, Sanjeev Krishna1,2,7,11, Peter G Kremsner1,2,3.   

Abstract

BACKGROUND: The rVSVΔG-ZEBOV-GP vaccine prevented Ebola virus disease when used at 2 × 107 plaque-forming units (PFU) in a trial in Guinea. This study provides further safety and immunogenicity data. METHODS AND
FINDINGS: A randomised, open-label phase I trial in Lambaréné, Gabon, studied 5 single intramuscular vaccine doses of 3 × 103, 3 × 104, 3 × 105, 3 × 106, or 2 × 107 PFU in 115 adults and a dose of 2 × 107 PFU in 20 adolescents and 20 children. The primary objective was safety and tolerability 28 days post-injection. Immunogenicity, viraemia, and shedding post-vaccination were evaluated as secondary objectives. In adults, mild-to-moderate adverse events were frequent, but there were no serious or severe adverse events related to vaccination. Before vaccination, Zaire Ebola virus (ZEBOV)-glycoprotein (GP)-specific and ZEBOV antibodies were detected in 11% and 27% of adults, respectively. In adults, 74%-100% of individuals who received a dose 3 × 104, 3 × 105, 3 × 106, or 2 × 107 PFU had a ≥4.0-fold increase in geometric mean titres (GMTs) of ZEBOV-GP-specific antibodies at day 28, reaching GMTs of 489 (95% CI: 264-908), 556 (95% CI: 280-1,101), 1,245 (95% CI: 899-1,724), and 1,503 (95% CI: 931-2,426), respectively. Twenty-two percent of adults had a ≥4-fold increase of ZEBOV antibodies, with GMTs at day 28 of 1,015 (647-1,591), 1,887 (1,154-3,085), 1,445 (1,013-2,062), and 3,958 (2,249-6,967) for the same doses, respectively. These antibodies persisted up to day 180 for doses ≥3 × 105 PFU. Adults with antibodies before vaccination had higher GMTs throughout. Neutralising antibodies were detected in more than 50% of participants at doses ≥3 × 105 PFU. As in adults, no serious or severe adverse events related to vaccine occurred in adolescents or children. At day 2, vaccine RNA titres were higher for adolescents and children than adults. At day 7, 78% of adolescents and 35% of children had recombinant vesicular stomatitis virus RNA detectable in saliva. The vaccine induced high GMTs of ZEBOV-GP-specific antibodies at day 28 in adolescents, 1,428 (95% CI: 1,025-1,989), and children, 1,620 (95% CI: 806-3,259), and in both groups antibody titres increased up to day 180. The absence of a control group, lack of stratification for baseline antibody status, and imbalances in male/female ratio are the main limitations of this study.
CONCLUSIONS: Our data confirm the acceptable safety and immunogenicity profile of the 2 × 107 PFU dose in adults and support consideration of lower doses for paediatric populations and those who request boosting. TRIAL REGISTRATION: Pan African Clinical Trials Registry PACTR201411000919191.

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Year:  2017        PMID: 28985239      PMCID: PMC5630143          DOI: 10.1371/journal.pmed.1002402

Source DB:  PubMed          Journal:  PLoS Med        ISSN: 1549-1277            Impact factor:   11.069


Introduction

The western African Ebola virus disease (EVD) public health emergency of international concern ended in June 2016 [1], after infecting approximately 28,650 individuals, of whom 11,323 died [2,3]. Global commitment led to landmarks in vaccine development against EVD, with 8 candidates out of 15 undergoing evaluation in phase I–III clinical trials worldwide by the end of 2015 [4-6]. A live-attenuated recombinant vaccine consisting of the vesicular stomatitis virus (VSV), strain Indiana, with the gene for the Kikwit-95 Zaire Ebola virus (ZEBOV) glycoprotein (GP) replacing the VSV glycoprotein (G) had given acceptable results in non-human primate challenge models and was selected for accelerated clinical development. In European and African populations, the VEBCON Consortium (VSV-EBola CONsortium) carried out parallel dose-escalation phase I trials of the recombinant VSV (rVSV)–ZEBOV candidate vaccine in Germany (NCT02283099), Kenya (NCT02296983), and Gabon (PACTR2014000089322) and a double-blind phase I/II randomised controlled trial in Switzerland (NCT02287480). Three further phase II/III trials were later launched in Guinea, Sierra Leone, and Liberia. Results from phase I trials in the US [7] and preclinical data supported selection of the 2 × 107 plaque-forming units (PFU) dose as the most immunogenic for phase IIb/III trials in Guinea, Sierra Leone, and Liberia. A final analysis of the Guinea trial showed that a single dose of 2 × 107 PFU given immediately after contact with an index case was 100% (95% CI: 70%–100%, P = 0.0045) efficacious in preventing EVD in individuals, and protected the population through a ring vaccination strategy 10 days or more post-vaccination [8]. Detailed dose-ranging studies (3 × 105, 3 × 106, 1 × 107, 2 × 107, and 5 × 107 PFU) at the 4 VEBCON sites showed acceptable safety, dose-dependent reactogenicity [9], and high seroconversion rates among all participants on day 28 after vaccination [9,10]. In Gabon, 2 seroprevalence studies in epidemic and non-epidemic regions showed varying proportions of participants with pre-vaccination ZEBOV-specific IgG antibodies [11,12]. In Lambaréné, with no reported EVD outbreak, ZEBOV-GP-specific antibody responses after vaccination were similar at 2 tested doses (3 × 105 and 3 × 106 PFU) [9]. This finding contrasted with that in vaccinees in Geneva, where antibody titres at 3 × 105 PFU were significantly lower than responses to higher vaccine doses, including 1 × 107 PFU and 5 × 107 PFU [10]. Additionally, irrespective of vaccine dose, delayed oligoarthritis and skin and mucous membrane lesions emerged as vaccine-related adverse events in a proportion of recipients more than 1 week after vaccination in Geneva [10]. These delayed complications were not observed in Gabon, despite the fact that the same vaccine batch and similar doses were used [9]. Because of these divergent site-specific observations, we need further assessments of the vaccine in Ebola virus endemic areas as well as in children. We present a comparison of safety and immunogenicity outcomes in participants vaccinated with (1) 2 × 107 PFU, the dose used in the efficacy trial; (2) 2 previously reported doses, 3 × 106 and 3 × 105 PFU [9]; and (3) 2 lower doses, 3 × 104 PFU and 3 × 103 PFU, in African adults. Furthermore, we report, to our knowledge for the first time, on children and adolescents aged 6 to 17 years vaccinated with 2 × 107 PFU.

Methods

Study design and participants

The trial protocol was approved by the Scientific Review Committee of Centre de Recherches Médicales de Lambaréné (CERMEL), the Institutional Ethics Committee of CERMEL, the National Ethics Committee of Gabon, the World Health Organization (WHO) Ethics Committee, and the Institutional Ethics Committee of the Universitätsklinikum Tübingen. The trial was registered with the Pan African Clinical Trials Registry (PACTR201411000919191). The study was a randomised, open-label, dose-escalation phase I trial at CERMEL in Gabon. The trial was initially designed to escalate doses to 3 × 105, 3 × 106, and 2 × 107 PFU in 60 adults. After successive protocol amendments, a total of 115 adults (18–50 years), 20 adolescents (13–17 years), and 20 children (6–12 years) were enrolled, between 17 November 2014 and 7 July 2015. Written informed consent was obtained from adults and parents/guardians of adolescents/children, and written assent from minors aged 11–17 years, prior to study-related procedures (details are in S3 Text). Healthy consenting volunteers who were aged 6–50 years and resident in the study area—which had no history of an Ebola outbreak—and willing to minimise blood/body fluid exposure to their relatives for 5 days post-vaccination were included. Field workers used the door-to-door approach to invite individuals from the Lambaréné community to screen for the study. After screening, individuals with a history of severe local or systemic allergic reaction to vaccination, known allergy to constituents of the rVSVΔG-ZEBOV-GP vaccine, or any acute or chronic clinically significant medical or psychiatric condition were excluded. All pregnant and lactating women were excluded. Volunteers who received a licensed vaccine within 14 days (or 30 days for a live vaccine), had a history of blood donation within 60 days prior to vaccination, were positive for HIV and/or hepatitis B or C virus infection, or had an immunocompromised member in the family were also excluded from the study.

Randomisation and treatment allocation

Randomisation and allocation was performed by an independent investigator from 17 November 2014 until 13 April 2015 using a web-generated sequence. Randomisation in permuted blocks was performed in 2 stages. In the first, participants were assigned in a ratio of 1:1:1 to 3 × 105, 3 × 106, and 2 × 107 PFU, and in the second stage, in a ratio of 1:1 to 3 × 103 and 3 × 104 PFU. On 9 December 2014, a temporary consortium-wide safety hold was placed on doses above 1 × 107 PFU due to adverse events reported at the Swiss site with doses of 1 × 107 and 5 × 107 PFU. In Gabon, only 1 participant had been allocated to the 2 × 107 PFU dose. In all, 20, 20, 1, 20, and 20 adults were randomised to a vaccine dose of 3 × 105, 3 × 106, 2 × 107, 3 × 103, and 3 × 104 PFU, respectively. Preliminary data from the 20 participants vaccinated with 3 × 105 PFU and the initial 19 vaccinated with 3 × 106 PFU were previously reported [9]. An unblinded safety review of VEBCON Consortium trials by the data and safety monitoring board lifted the safety hold on 5 January 2015. After this and during the third stage of the study, 19 adults were vaccinated with 3 × 106 PFU without randomisation. In addition, Merck Sharp & Dohme selected the 2 × 107 PFU dose for further development, as being the most immunogenic dose with an acceptable safety profile (S. Gupta, oral presentation at the WHO Ebola Research and Development Summit, 11–12 May 2015, Geneva) [13,14]. A subsequent amendment included 20 adolescents and 20 children aged 13 to 17 years and 6 to 12 years, respectively, to be vaccinated with 2 × 107 PFU. The National Ethics Committee of Gabon recommended that adults from this population should be vaccinated with the intended dose before administration to the paediatric cohorts, so an additional 15 adults were included in the study (S3 Text).

Vaccine and vaccination procedures

The rVSVΔG-ZEBOV-GP vaccine, developed by the Canadian National Laboratory under the patent number WO2004011488 A2 and licensed to BioProtection Systems (NewLink Genetics), was the unique intervention in this trial. The vaccine was subsequently sublicensed to Merck and was manufactured at IDT Biologika (Dessau-Rosslau, Germany). WHO supplied single-dose vials of 1 × 108 PFU (lot no 0030513) to conduct the trial at CERMEL, from a donation of rVSVΔG-ZEBOV-GP by the Canadian government to WHO. The dispensed vials were reconstituted in serial dilutions for vaccination. A single injection of 1 ml of the reconstituted vaccine for the required dose was administered intramuscularly into the deltoid muscle of volunteers at vaccination (S1 Fig).

Safety assessments

The nature, frequency, and severity of adverse events constituted the primary safety endpoint of the trial. Local and systemic reactogenicity symptoms and signs (solicited adverse events) were recorded for 14 days post-injection. Unsolicited adverse events, including laboratory anomalies, were recorded up to 28 days post-injection. Detailed descriptions of all serious adverse events were recorded throughout the study follow-up visits, as a secondary safety endpoint. Solicited adverse events (pain, swelling, redness) were obtained by direct examination of the injection site, or direct questioning when follow-up occurred by telephone. Arthralgia and arthritic symptoms were later added as a solicited adverse event upon the request of the data and safety monitoring board. Participants were asked specifically if they were experiencing these symptoms.

rVSVΔG-ZEBOV-GP viraemia and shedding

Plasma, saliva, and urine samples (at screening and days 1, 2, and 7 post-vaccination) were processed and stored in Trizol LS at the study site, until rVSVΔG-ZEBOV-GP viral load determinations were performed by reverse transcriptase quantitative PCR as a secondary outcome. The lower limit of detection for rVSVΔG-ZEBOV-GP RNA was 30 copies/ml, and the lower level of quantification was 100 copies/ml [9].

Immunological assessments

As a secondary objective, enzyme-linked immunosorbent assays (ELISAs) were performed on days 0, 28, 56, 84, and 180 after injection. ZEBOV-specific antibody assays were conducted at the Institute for Virology, Marburg. Antibodies were detected using an antibody capture ELISA based on inactivated Ebola Zaire Makona virus particles [15]. ELISA for ZEBOV-GP-specific antibodies was performed at the US Army Medical Research Institute of Infectious Diseases (USAMRIID) using the Kikwit-95 ZEBOV strain GP (standard operating procedure AP-03-35-00). Antibodies were reported as geometric mean titres (GMTs), or geometric mean concentrations, of arbitrary ELISA units (AEU) per millilitre with 95% confidence intervals, as indicated. Neutralising antibodies (Nabs) were detected using either particles of Ebola virus (Zaire isolate Mayinga, AF086833), with the assays being performed in a BSL4 laboratory (Institute for Virology, Marburg), or VSV pseudovirions expressing the luciferase reporter gene complemented by GP from the Kikwit-95 ZEBOV strain, with assays being performed at USAMRIID. All 4 assays were previously reported by our team [9,15] and other researchers working on this candidate vaccine in the US [7].

Statistical analysis

WHO estimated that a sample size of 74–124 participants would be needed across the VEBCON Consortium sites to show a 2-fold change in ZEBOV-specific antibody titres between vaccine doses and proposed a target sample size of approximately 250 participants for all sites [10]. We described the frequency and intensity of adverse events using counts and percentages, means and standard deviations, or medians and interquartile ranges (IQRs), for skewed continuous variables. Chi-squared test or Fisher’s exact test was used to compare pairwise proportions. Seropositivity rates were defined as the percentage of participants having AEU above a cutoff per vaccine group. Seroconversion rates were defined as the percentage of converted participants in each group. McNemar’s test was used to compare the seropositivity between day 0 and other days. We used Fisher’s test to perform inter-group comparisons and to determine the association between the seroconversion rate and seropositivity rate at each time point. Antibody concentrations or units were normalised using log transformations, and responses are reported as GMTs with 95% confidence intervals or geometric mean of AEU per millilitre with 95% confidence intervals. Student’s test or Wilcoxon’s paired test was used to compare magnitudes of antibody induced between day 0 and other days. All statistical analyses were conducted in R statistical software version 3.1.2 [16], except for viraemias (copies/millilitre of plasma), which were analysed with a Kruskal–Wallis test combined with Dunn’s multiple comparison test using GraphPad Prism version 6.

Results

From 21 November 2014 to 13 April 2015, 115 adults were vaccinated with a single injection of rVSVΔG-ZEBOV-GP at 5 different doses. Twenty adolescents and 20 children were vaccinated between 8 May and 7 July 2015 (Fig 1).
Fig 1

Participant flow diagram.

Randomisation and flow of participants over a period of 6 months for adults (cohorts 1 to 5), adolescents (cohort 6; 13–17 years), and children (cohort 7; 6–12 years). Similar dose groups are matched with shading (light grey, 3 × 106 PFU; dark grey, 2 × 107 PFU). GP, glycoprotein; ELISA, enzyme-linked immunosorbent assay; PFU, plaque-forming units; rVSV, recombinant vesicular stomatitis virus.

Participant flow diagram.

Randomisation and flow of participants over a period of 6 months for adults (cohorts 1 to 5), adolescents (cohort 6; 13–17 years), and children (cohort 7; 6–12 years). Similar dose groups are matched with shading (light grey, 3 × 106 PFU; dark grey, 2 × 107 PFU). GP, glycoprotein; ELISA, enzyme-linked immunosorbent assay; PFU, plaque-forming units; rVSV, recombinant vesicular stomatitis virus. Safety and immunogenicity data are reported until month 6 for adults, adolescents, and children for all 155 participants. In all, 108 (93%) adults and 36 (90%) adolescents and children attended all planned immunogenicity visits. Mean age and body mass index were similar among the 5 adult cohorts, with 21 adult women enrolled in the trial (Table 1).
Table 1

Baseline characteristics of study participants.

CharacteristicAdults (18–50 years)Adolescents (13–17 years): 2 × 107 PFU (N = 20)Children (6–12 years): 2 × 107 PFU (N = 20)
3 × 103 PFU (N = 20)3 × 104 PFU (N = 20)3 × 105 PFU*(N = 20)3 × 106 PFU*(N = 39)2 × 107 PFU (N = 16)
Sex, n (percent)
Male13 (65)17 (85)14 (70)35 (90)15 (94)19 (95)16 (80)
Female7 (35)3 (15)6 (30)4 (10)1 (6)1 (5)4 (2)
Age (years), mean (SD)27 (8)23 (5)28 (7)27 (7)25 (6)15 (1)9 (1)
BMI (kg/m2), mean (SD)23 (3)23 (3)23 (3)23 (3)23 (2)18 (2)16 (1)

*Already reported in The New England Journal of Medicine (doi: 10.1056/NEJMoa1502924) [9]: 3 × 105 PFU, N = 20, and 3 × 106 PFU, N = 19.

BMI, body mass index; PFU, plaque-forming units.

*Already reported in The New England Journal of Medicine (doi: 10.1056/NEJMoa1502924) [9]: 3 × 105 PFU, N = 20, and 3 × 106 PFU, N = 19. BMI, body mass index; PFU, plaque-forming units.

Assessment of 5 vaccine doses in adult volunteers

Reactogenicity and tolerability

Headaches, fatigue, pain at injection site, gastrointestinal symptoms, and subjective fever were the most frequent symptoms. Of these, 68% were mild and 32% moderately intense, with similar frequencies up to day 28 across cohorts in adults. There were no vaccine-related severe adverse events (Tables 2 and S1).
Table 2

Reactogenicity to rVSVΔG-ZEBOV-GP vaccine until day 28 post-vaccination.

Adverse events/gradingNumber (percent) of participants
AdultsChildren: 2 × 107 PFU (N = 20)Adolescents: 2 × 107 PFU (N = 20)
3 × 103 PFU (N = 20)3 × 104 PFU (N = 20)3 × 105 PFU* (N = 20)3 × 106 PFU* (N = 39)2 × 107 PFU (N = 16)
Adverse events (highest grade)
None6# (30%)8 (40%)2 (10%)5 (13%)1 (6%)0 (0%)0 (0%)
Mild9# (45%)7 (35%)11 (55%)20 (51%)10 (63%)15 (75%)14 (70%)
Moderate5 (25%)5 (25%)7 (35%)14 (36%)5 (31%)5 (25%)6 (30%)
Solicited injection site reactions
Pain
None17 (85%)16 (80%)17 (85%)17 (44%)7 (44%)9 (45%)10 (50%)
Mild3 (15%)3 (15%)3 (15%)22 (56%)6 (37%)9 (45%)8 (40%)
Moderate0 (0%)1 (5%)0 (0%)0 (0%)3 (19%)2 (10%)2 (10%)
Swelling
None20 (100%)20 (100%)20 (100%)39 (100%)15 (94%)20 (100%)19 (95%)
Mild0 (0%)0 (0%)0 (0%)0 (0%)1 (6%)0 (0%)1 (5%)
Solicited systemic reactions
Headache
None11 (55%)15 (75%)11 (55%)17 (44%)8 (50%)10 (50%)7 (35%)
Mild6 (30%)4 (20%)6 (30%)14 (36%)6 (37%)9 (45%)10 (50%)
Moderate3 (15%)1 (5%)3 (15%)8 (20%)2 (13%)1 (5%)3 (15%)
Myalgia
None17 (85%)18 (90%)18 (90%)29 (74%)14 (87%)16 (80%)14 (70%)
Mild2 (10%)1 (5%)1 (5%)6 (15%)2 (13%)3 (15%)5 (25%)
Moderate1 (5%)1 (5%)1 (5%)4 (10%)0 (0%)1 (5%)1 (5%)
Subjective fever
None18 (90%)15 (75%)19 (95%)28 (72%)9 (56%)12 (60%)12 (60%)
Mild1 (5%)3 (15%)1 (5%)9 (23%)7 (44%)7 (35%)7 (35%)
Moderate1 (5%)2 (10%)0 (0%)2 (5%)0 (0%)1 (5%)1 (5%)
Fatigue
None16 (80%)14 (70%)10 (50%)20 (51%)12 (75%)10 (50%)13 (65%)
Mild3 (15%)5 (25%)7 (35%)11 (28%)3 (19%)8 (40%)3 (15%)
Moderate1 (5%)1 (5%)3 (15%)8 (20%)1 (6%)2 (10%)4 (20%)
Objective fever
None17 (85%)19 (95%)19 (95%)33 (85%)12 (75%)13 (65%)15 (75%)
Mild3 (15%)1 (5%)1 (5%)3 (8%)4 (25%)7 (35%)5 (25%)
Moderate0 (0%)0 (0%)0 (0%)3 (8%)0 (0%)0 (0%)0 (0%)
Gastrointestinal symptoms
None17 (85%)13 (65%)10 (50%)28 (72%)10 (63%)8 (40%)14 (70%)
Mild3 (15%)6 (30%)7 (35%)10 (26%)6 (38%)10 (50%)3 (15%)
Moderate0 (0%)1 (5%)3 (15%)1 (3%)0 (0%)2 (10%)3 (15%)
Chills
None20 (100%)20 (100%)20 (100%)35 (90%)16 (100%)15 (75%)17 (85%)
Mild0 (0%)0 (0%)0 (0%)4 (10%)0 (0%)5 (25%)3 (15%)
Arthralgia
None17 (85%)17 (85%)18 (90.0%)26 (67%)12 (75%)17 (85%)16 (80%)
Mild0 (0%)0 (0%)0 (0%)8 (21%)1 (6%)2 (10%)3 (15%)
Moderate3 (15%)3 (15%)2 (10%)5 (13%)3 (19%)1 (5%)1 (5%)
Mouth ulcer
None20 (100%)20 (100%)19 (95%)37 (95%)14 (88%)18 (90%)20 (100%)
Mild0 (0%)0 (0%)1 (5%)2 (5%)1 (6%)1 (5%)0 (0%)
Moderate0 (0%)0 (0%)0 (0%)0 (0%)1 (6%)1 (5%)0 (0%)
Skin lesion
None20 (100%)19 (95%)19 (95%)38 (97%)11 (69%)19 (95%)18 (90%)
Mild0 (0%)1 (5%)1 (5%)0 (0%)4 (25%)1 (5%)2 (10%)
Moderate0 (0%)0 (0%)0 (0%)1 (3%)1 (6%)0 (0%)0 (0%)
Blister
None20 (100%)20 (100%)20 (100%)39 (100%)15 (94%)20 (100%)20 (100%)
Mild0 (0%)0 (0%)0 (0%)0 (0%)1 (6%)0 (0%)0 (0%)
Unsolicited adverse events
Malaria
None19 (95%)20 (100%)15 (75%)36 (92%)8 (50%)18 (90%)17 (85%)
Mild1 (5%)0 (0%)0 (0%)0 (0%)4 (25%)0 (0%)2 (10%)
Moderate0 (0%)0 (0%)5 (25%)3 (8%)4 (25%)2 (10%)1 (5%)
Rhinitis
None18 (90%)19 (95%)18 (90%)38 (97%)12 (75%)19 (95%)17 (85%)
Mild2 (10%)1 (5%)2 (10%)1 (3%)4 (25%)1 (5%)3 (15%)
Cough
None14 (70%)17 (85%)20 (100%)39 (100%)12 (75%)17 (85%)20 (100%)
Mild3 (15%)2 (10%)0 (0%)0 (0%)4 (25%)2 (10%)0 (0%)
Moderate3 (15%)1 (5%)0 (0%)0 (0%)0 (0%)1 (5%)0 (0%)
Other
None14 (70%)11 (55%)3 (15%)17 (44%)0 (0%)10 (50%)14 (70%)
Mild2 (10%)4 (20%)10 (50%)13 (33%)17 (68%)8 (40%)6 (30%)
Moderate4 (20%)5 (25%)7 (35%)9 (23%)8 (32%)2 (10%)0 (0%)

*Already reported in The New England Journal of Medicine (doi: 10.1056/NEJMoa1502924) [9]: 3 × 105 PFU, N = 20, and 3 × 106 PFU, N = 19.

#Total number of participants reporting at least 1 event within 28 days after vaccination with rVSVΔG-ZEBOV-GP vaccine. Only events with the highest grade are reported per cohort.

PFU, plaque-forming units.

*Already reported in The New England Journal of Medicine (doi: 10.1056/NEJMoa1502924) [9]: 3 × 105 PFU, N = 20, and 3 × 106 PFU, N = 19. #Total number of participants reporting at least 1 event within 28 days after vaccination with rVSVΔG-ZEBOV-GP vaccine. Only events with the highest grade are reported per cohort. PFU, plaque-forming units. Monocytes increased and lymphocytes decreased in the first week after vaccination in a dose-dependent fashion (S5 Table). Mild-to-moderate symptoms reported at days 56, 84, and 180 and during unscheduled visits were considered unrelated to the study vaccine (S4 Table). Few haematological or biochemical changes of clinical significance were captured as adverse events, and these were followed up until resolution without sequelae. A total of 11 adult participants experienced a serious adverse event. Six participants had malaria requiring hospitalisation, 2 underwent surgery due to appendicitis, and 1 was diagnosed with glaucoma. The last probably had the condition prior to enrolment after a detailed history was obtained, and is now receiving specialised care. Two individuals were hospitalised for bleeding after dental surgery and gastritis, respectively. All of these events were judged unrelated to the vaccine. Three women became pregnant after vaccination; they were monitored until delivery. Their neonates had no safety complications.

Immunogenicity

Eleven adults were excluded from either sampling and/or analysis of immunogenicity data: a male participant was HIV positive, 3 women became pregnant beyond day 28 after vaccination, and 7 participants received anti-tetanus vaccine/immunoglobulin. These participants were not sampled on subsequent visits (days 56, 84, and 180).

ZEBOV-GP-specific and ZEBOV antibodies

In all, 70%–100% of adult participants vaccinated with all doses ≥3 × 104 PFU reached a greater than 4.0-fold increase of ZEBOV-GP-specific GMT at day 28. ZEBOV-GP antibody GMTs peaked at day 56, with antibody levels persistently higher than baseline up to 6 months post-vaccination (Table 3).
Table 3

Endpoint geometric mean titres, seropositivity rates, and proportions of seroresponders to rVSVΔG-ZEBOV-GP measured by ZEBOV-GP ELISA in adults.

DoseTime*NGMT (95% CI)Seropositivity (>200 AEU/ml), N (percent)Seroresponse (≥4×), N (percent)P value
Early change in GMTChange in seropositivitySeropositivity and seroresponseLater change in GMTβ
3 × 103 PFUD02024 (9–60)4 (20)0 (0)
D281981 (35–184)5 (26)7 (37)0.0810.030.5
D561843 (14–131)5 (28)8 (44)0.310.0060.5
3 × 104 PFUD02023 (9–63)2 (10)0 (0)
D2819489 (264–908)14 (74)16 (84)<0.0010.0010.01
D5616633 (305–1,314)14 (88)15 (94)<0.0010.0010.1
3 × 105 PFUD01910 (4–22)0 (0)0 (0)
D2820556 (280–1,101)15 (75)18 (90)<0.001<0.0010.050.1
D5617676 (246–1,859)13 (77)15 (88)<0.0010.0010.040.01
D8417536 (215–1,338)14 (82)15 (882)<0.001<0.0010.020.01
D18016365 (187–713)12 (75)15 (94)<0.0010.0020.2
3 × 106 PFUD03916 (9–27)3 (8)0 (0)
D28391,245 (899–1,724)39 (100)39 (100)<0.001<0.0011<0.001
D56371,331 (977–1,813)36 (973)37 (100)<0.001<0.0011<0.001
D8435994 (731–1,352)33 (943)35 (100)<0.001<0.0011<0.001
D18037685 (546–858)35 (95)36 (97)<0.001<0.0010.05
2 × 107 PFUD01647 (19–115)4 (25)0 (0)
D28161,503 (931–2,426)16 (100)16 (100)<0.0010.00110.3
D56132,590 (1,604–4,182)13 (100)12 (92)<0.0010.00710.004
D84141,826 (1,134–2,940)14 (100)13 (93)<0.0010.00410.09
D180151,514 (997–2,301)15 (100)15 (100)<0.0010.0021

ZEBOV-GP-specific antibodies are expressed in GMTs with 95% confidence intervals. Seropositivity is defined by geometric mean concentration > 200 AEU/ml. Seroresponse is defined by a ≥4-fold rise in GMT. P values < 0.05 are given in bold.

*Time point in day(s) since vaccination.

†Wilcoxon’s test for paired data. P < 0.05 indicates a statistical difference in antibody titre between day 0 and other days.

‡McNemar’s test. P < 0.05 indicates a statistical difference in seropositivity rate between day 0 and other days (28, 56, and 84 days post-vaccination).

ΩFisher’s test. P < 0.05 indicates a statistical association between seropositivity and seroresponse for each time point.

βWilcoxon’s test for paired data. P < 0.05 indicates a statistical difference in antibody titre between day 180 post-vaccination and days 28, 56, and 84 post-vaccination.

AEU, arbitrary enzyme-linked immunosorbent assay units; ELISA, enzyme-linked immunosorbent assay; GMT, geometric mean titre; PFU, plaque-forming units; ZEBOV, Zaire Ebola virus.

ZEBOV-GP-specific antibodies are expressed in GMTs with 95% confidence intervals. Seropositivity is defined by geometric mean concentration > 200 AEU/ml. Seroresponse is defined by a ≥4-fold rise in GMT. P values < 0.05 are given in bold. *Time point in day(s) since vaccination. †Wilcoxon’s test for paired data. P < 0.05 indicates a statistical difference in antibody titre between day 0 and other days. ‡McNemar’s test. P < 0.05 indicates a statistical difference in seropositivity rate between day 0 and other days (28, 56, and 84 days post-vaccination). ΩFisher’s test. P < 0.05 indicates a statistical association between seropositivity and seroresponse for each time point. βWilcoxon’s test for paired data. P < 0.05 indicates a statistical difference in antibody titre between day 180 post-vaccination and days 28, 56, and 84 post-vaccination. AEU, arbitrary enzyme-linked immunosorbent assay units; ELISA, enzyme-linked immunosorbent assay; GMT, geometric mean titre; PFU, plaque-forming units; ZEBOV, Zaire Ebola virus. About 11% (13/114) of adult participants had ZEBOV-GP-specific ELISA antibody concentrations > 200 AEU/ml at baseline. The proportions of individuals with high concentrations at baseline were inconsistent across vaccine groups and ranged from 0% to 25%. Antibody concentrations were significantly higher at day 56 post-vaccination in individuals with prior antibodies following vaccination with doses of 3 × 103, 3 × 104, and 3 × 106 PFU (Table 4).
Table 4

Endpoint geometric mean titres measured by USAMRIID ZEBOV-GP ELISA in adults with and without baseline specific antibodies.

DoseTime *With baseline GP-specific antibodiesWithout baseline GP-specific antibodiesP value
NGMT (95% CI)NGMT (95% CI)
3 × 103 PFUD04346 (244–492)1612 (59–30)0.002
D284305 (157–592)1557 (22–148)0.08
D564295 (157–554)1425 (7–90)0.04
3 × 104 PFUD02549 (328–919)1816 (6–43)0.02
D2823,489 (1,083–11,245)17388 (215–701)0.04
D5625,229 (2,435–11,232)14468 (234–937)0.03
3 × 105 PFUD01910 (4–22)
D2820556 (280–1,101)
D5617676 (246–1,859)
D8417536 (215–1,338)
D18016365 (187–713)
3 × 106 PFUD03310 (181–532)3612 (7–20)0.004
D2836,307 (1,125–35,368)361,088 (813–1,454)0.06
D5634,263 (1,885–9,640)341,201 (882–1,634)0.01
D8432,984 (1,720–5,175)32897 (657–1,223)0.004
D18031,616 (1,225–2,133)34635 (505–797)0.004
2 × 107 PFUD04375 (223–632)1223 (10–56)<0.001
D2841,466 (761–2,824)121,516 (820–2,801)0.8
D5642,174 (1,713–2,760)92,799 (1,401–5,590)0.7
D8441,514 (882–2,597)101,968 (1,036–3,738)0.6
D18041,013 (672–1,526)111,753 (1,028–2,990)0.1

Seropositivity at day 0 (D0) defined by a GMT > 200 AEU/ml. P values < 0.05 are given in bold.

*Time point in day(s) since vaccination.

†Wilcoxon’s test. P < 0.05 indicates a statistical difference in antibody titre at each time point between the adults with and without the antibodies at D0.

AEU, arbitrary enzyme-linked immunosorbent assay units; ELISA, enzyme-linked immunosorbent assay; GMT, geometric mean titre; GP, glycoprotein; PFU, plaque-forming units; USAMRIID, US Army Medical Research Institute of Infectious Diseases; ZEBOV, Zaire Ebola virus.

Seropositivity at day 0 (D0) defined by a GMT > 200 AEU/ml. P values < 0.05 are given in bold. *Time point in day(s) since vaccination. †Wilcoxon’s test. P < 0.05 indicates a statistical difference in antibody titre at each time point between the adults with and without the antibodies at D0. AEU, arbitrary enzyme-linked immunosorbent assay units; ELISA, enzyme-linked immunosorbent assay; GMT, geometric mean titre; GP, glycoprotein; PFU, plaque-forming units; USAMRIID, US Army Medical Research Institute of Infectious Diseases; ZEBOV, Zaire Ebola virus. The whole-virion assay is a less sensitive method to detect vaccine-induced antibody responses, which are directed against GP; 34% and 63% of vaccinees who received a dose equal to or more than 3 × 105 PFU reached a greater than 2.0-fold increase in ZEBOV antibody GMT at day 28 and 56, respectively. Only 40% (30/74) of participants in the dose groups 3 × 105, 3 × 106, and 2 × 107 PFU had a greater than 2.0-fold increase in antibody persisting up to 6 months post-injection (Table 5).
Table 5

Geometric mean titres, seropositivity rates, and proportions of seroresponders to rVSVΔG-ZEBOV-GP measured by whole-virion ELISA in adults.

DoseTime point*NGMT (95% CI)Seropositivity (>500 AEU/ml), N (percent)Seroresponse, N (percent)P value
≥2×≥4×Change in GMTChange in seropositivitySeropositivity and seroresponse (≥2×)Seropositivity and seroresponse (≥4×)β
3 × 103 PFUD020718 (529–975)5 (25)
D2820673 (975–896)4 (20)0 (0)0 (0)0.2811
D5618803 (565–1,141)6 (33)1 (60 (0)0.400.331
3 × 104 PFUD020949 (627–1,435)7 (35)
D28201,015 (647–1,591)7 (35)1 (5)0 (0)0.200.351
D56161,029 (628–1,686)5 (31)1 (6)0 (0)0.400.310.31
3 × 105 PFUD019575 (440–751)1 (5)
D720641 (481–851)3 (15)2 (11)0 (0)0.420.470.021
D1418674 (502–905)4 (22)2 (12)1 (6)0.580.240.041
D28201,887 (1,154–30,853)13 (65)11 (58)10 (53)0.010.002<0.001<0.001
D56171,402 (842–2,333)8 (47)7 (44)7 (440.020.02<0.001<0.001
D84171,667 (1,098–2,531)12 (71)10 (63)6 (38)0.030.0040.0010.09
D180161,194 (809–1,762)9 (56)5 (33)5 (33)0.180.020.020.02
3 × 106 PFUD039693 (565–850)9 (23)
D738726 (573–920)8 (21)2 (5)0 (0)0.1810.041
D14381,037 (734–1,463)15 (40)11 (29)4 (11)0.0030.07<0.0010.01
D28391,445 (1,013–2,062)21 (54)17 (44)11 (28)<0.0010.001<0.001<0.001
D56371,824 (1,316–2,527)27 (73)24 (65)10 (27)<0.001<0.001<0.0010.03
D84361,586 (1,179–2,133)25 (69)19 (53)8 (22)<0.001<0.001<0.0010.07
D180381,450 (1,105–1,903)26 (68)19 (50)7 (18)<0.001<0.001<0.0010.07
2 × 107 PFUD0161,625 (879–3,006)9 (56)
D7161,220 (695–2,142)7 (44)0 (0)0 (0)0.010.4711
D14162,153 (1,140–4,067)10 (63)2 (13)1 (6)0.1610.51
D28163,958 (2,249–6,967)13 (81)7 (44)4 (25)0.0030.220.210.5
D56134,402 (2,888–6,711)12 (92)6 (46)4 (31)0.0020.2211
D84143,638 (2,372–5,580)13 (93)7 (50)3 (21)0.010.1311
D180152,963 (1,769–4,962)13 (87)6 (40)3 (20)0.30.220.481

ZEBOV antibodies are expressed in GMTs with 95% confidence intervals. Seropositivity is defined by a GMT > 500 AEU/ml. Seroresponse is expressed as a ≥2-fold or ≥4-fold increase in titre. P values < 0.05 are given in bold.

*Time point in day(s) since vaccination.

†Wilcoxon’s test for paired data. P < 0.05 indicates a statistically significant difference in antibody titre between day 0 and other days.

‡McNemar’s test. P < 0.05 indicates a statistically significant difference in seropositivity rate between day 0 and other days.

ΩFisher’s test. P < 0.05 indicates a statistical association between seropositivity and seroresponse (≥2×) for each time point.

βFisher’s test. P < 0.05 indicates a statistical association between seropositivity and seroresponse (≥4×) for each time point.

AEU, arbitrary enzyme-linked immunosorbent assay units; ELISA, enzyme-linked immunosorbent assay; GMT, geometric mean titre; PFU, plaque-forming units.

ZEBOV antibodies are expressed in GMTs with 95% confidence intervals. Seropositivity is defined by a GMT > 500 AEU/ml. Seroresponse is expressed as a ≥2-fold or ≥4-fold increase in titre. P values < 0.05 are given in bold. *Time point in day(s) since vaccination. †Wilcoxon’s test for paired data. P < 0.05 indicates a statistically significant difference in antibody titre between day 0 and other days. ‡McNemar’s test. P < 0.05 indicates a statistically significant difference in seropositivity rate between day 0 and other days. ΩFisher’s test. P < 0.05 indicates a statistical association between seropositivity and seroresponse (≥2×) for each time point. βFisher’s test. P < 0.05 indicates a statistical association between seropositivity and seroresponse (≥4×) for each time point. AEU, arbitrary enzyme-linked immunosorbent assay units; ELISA, enzyme-linked immunosorbent assay; GMT, geometric mean titre; PFU, plaque-forming units. About 27% (31/115) of adults had ZEBOV antibody concentrations > 500 AEU/ml at baseline, with inconsistent frequencies (5% to 56%) across dose levels. In adults with pre-vaccination antibodies, a dose as low as 3 × 104 PFU yielded a 2-fold increase in ZEBOV antibodies post-injection. Regardless of baseline status, the highest antibody titres were observed with the 2 × 107 PFU dose (Table 6).
Table 6

Geometric mean titres of ZEBOV antibodies in adults by baseline antibody status measured by whole-virion ELISA.

DoseTime*With baseline ZEBOV antibodiesWithout baseline ZEBOV antibodies
NGMT (95% CI)P valueNGMT (95% CI)P value
3 × 103 PFUD052,129 (1,276–3,552)15500 (—)
D2851,637 (780–3,435)0.3115500 (—)
D5652,196 (1,064–4,532)0.8113545 (466–638)
3 × 104 PFUD073,119 (2,106–4,621)13500 (—)
D2873,778 (2,642–5,403)0.2213500 (—)
D5663,428 (1,618–7,260)0.4310500 (—)
3 × 105 PFUD017,085 (—)18500 (—)
D716,325 (—)19567 (479–672)0.37
D1416,110 (—)17592 (495–708)0.18
D2814,372 (—)191,805 (1,084–3,007)0.003
D56171,402 (831–2,364)0.02
D8413,977 (—)161,579 (1,027–2,427)0.006
D18012,587 (—)151,134 (758–1,695)0.02
3 × 106 PFUD092,055 (1,458–2,896)30500 (—)
D792,108 (1,184–3,753)0.3029521 (481–565)1
D1494,129 (1,986–8,585)0.0429675 (534–854)0.02
D2894,686 (2,905–7,559)0.01301,015 (714–1,445)0.002
D5693,936 (2,009–7,711)0.02281,424 (1,021–1,987)<0.001
D8493,371 (1,834–6,196)0.04271,234 (920–1,654)<0.001
D18093,046 (1,758–5,276)0.07291,152 (882–1,504)<0.001
2 × 107 PFUD094,065 (2,274–7,266)7500 (—)
D792,440 (1,180–5,048)0.0077500 (—)
D1494,422 (2,339–8,361)0.427854 (383–1,900)0.37
D2895,633 (2,973–1,067)0.0572,515 (977–6,470)0.06
D5684,365 (2,286–8,332)0.0754,463 (2,634–7,561)0.06
D8484,179 (2,169–8,054)0.3163,024 (1,792–5,102)0.03
D18093,691 (1,877–7,255)0.5062,131 (956–4,752)0.06

Results are expressed in GMTs of AEU/millilitre with 95% confidence intervals. Seropositivity is defined by a GMT > 500 AEU/ml. Values below the threshold were given arbitrary units of 500 AEU/ml. P values < 0.05 are given in bold.

*Time point in day(s) since vaccination.

†Wilcoxon’s test for paired data used to compare antibody titres between time points; a P value < 0.05 indicates a statistically significant difference in antibody titre between day 0 and other days (D7, D14, D28, D56, D84, and D180). Samples from D84 for doses 3 × 103 and 3 × 104 PFU were not analysed.

AEU, arbitrary enzyme-linked immunosorbent assay units; ELISA, enzyme-linked immunosorbent assay; GMT, geometric mean titre; PFU, plaque-forming units; ZEBOV, Zaire Ebola virus.

Results are expressed in GMTs of AEU/millilitre with 95% confidence intervals. Seropositivity is defined by a GMT > 500 AEU/ml. Values below the threshold were given arbitrary units of 500 AEU/ml. P values < 0.05 are given in bold. *Time point in day(s) since vaccination. †Wilcoxon’s test for paired data used to compare antibody titres between time points; a P value < 0.05 indicates a statistically significant difference in antibody titre between day 0 and other days (D7, D14, D28, D56, D84, and D180). Samples from D84 for doses 3 × 103 and 3 × 104 PFU were not analysed. AEU, arbitrary enzyme-linked immunosorbent assay units; ELISA, enzyme-linked immunosorbent assay; GMT, geometric mean titre; PFU, plaque-forming units; ZEBOV, Zaire Ebola virus.

Neutralising antibodies

Nabs for doses of 3 × 104, 3 × 105, 3 × 106, and 2 × 107 were detected in 52%, 55%, 82%, and 62% of recipients against VSV-based Ebola pseudovirions (pseudovirion neutralisation assay 50% [PsVNA50]), respectively, and in 70%, 84%, and 56% of recipients against ZEBOV virus particles. The highest Nab GMTs were observed in recipients of 2 × 107 PFU. About 35%, 13%, and 25% of participants in the dose groups 3 × 105, 3 × 106, and 2 × 107 PFU, respectively, had baseline Nabs against ZEBOV virus particles (defined as GMT > GMT + SD at D0). Higher Nab GMTs were observed at day 28 regardless of baseline antibody status (Tables 7, S8 and S9).
Table 7

Geometric mean titres, seropositivity rates, and proportions of seroresponders to rVSVΔG-ZEBOV-GP measured by ZEBOV PsVNA50 in adults.

DoseTime point*NGMT (95% CI)Seropositivity (>20 titre), N (percent)Seroresponse (≥4×), N (percent)P value
Change in GMTChange in concentrationChange in seropositivity
3 × 103 PFUD01919 (—)0 (0)0 (0)
D281924 (19–32)3 (16)2 (11)0.10.20.01
3 × 104 PFUD01919 (—)0 (0)0 (0)
D281970 (36–135)10 (53)8 (42)0.0050.0040.001
3 × 105 PFUD01919 (—)0 (0)0 (0)
D282066 (34–128)11 (55)7 (35)0.0050.0040.004
D1801621 (17–27)1 (6)1 (6)110.06
3 × 106 PFUD03919 (—)0 (0)0 (0)
D283981 (56–119)32 (82)18 (46)<0.001<0.0010.009
D1803720 (19–22)6 (16)0 (0)0.030.041
2 × 107 PFUD01619 (—)0 (0)0 (0)
D2816126 (56–285)10 (63)10 (63)0.0050.004<0.001
D5613102 (52–202)9 (69)9 (69)0.0090.0070.001
D841430 (23–41)8 (57)1 (7)0.010.011
D1801526 (21–34)6 (40)1 (7)0.030.040.4

Results are expressed as geometric mean PsVNA50 neutralisation titres with 95 CIs. Seropositivity was defined as GMT > 20. Values below the threshold were given arbitrary titres of 19. Seroresponse was defined as a ≥4-fold increase. P values < 0.05 are given in bold.

*Time point in day(s) since vaccination.

†Wilcoxon’s test for paired data. P < 0.05 indicates a statistical difference in antibody titre between day 0 and other days.

‡McNemar’s test used to compare concentration between day 0 and other days. P value < 0.05 indicates a statistical difference in seropositivity rate between day 0 and other days.

ΩFisher’s test used to compare seropositivity rate between day 0 and each time point. P value < 0.05 indicates a statistical difference between tested time points.

GMT, geometric mean titre; PFU, plaque-forming units; PsVNA50, pseudovirion neutralisation assay 50%; ZEBOV, Zaire Ebola virus.

Results are expressed as geometric mean PsVNA50 neutralisation titres with 95 CIs. Seropositivity was defined as GMT > 20. Values below the threshold were given arbitrary titres of 19. Seroresponse was defined as a ≥4-fold increase. P values < 0.05 are given in bold. *Time point in day(s) since vaccination. †Wilcoxon’s test for paired data. P < 0.05 indicates a statistical difference in antibody titre between day 0 and other days. ‡McNemar’s test used to compare concentration between day 0 and other days. P value < 0.05 indicates a statistical difference in seropositivity rate between day 0 and other days. ΩFisher’s test used to compare seropositivity rate between day 0 and each time point. P value < 0.05 indicates a statistical difference between tested time points. GMT, geometric mean titre; PFU, plaque-forming units; PsVNA50, pseudovirion neutralisation assay 50%; ZEBOV, Zaire Ebola virus.

The vaccine dose of 2 × 107 PFU in adult, adolescent, and child volunteers

Twenty adolescents aged 13–17 years and 20 children aged 6–12 years were vaccinated with 1 intramuscular dose of 2 × 107 PFU. Adolescents and children reported mostly headaches, fatigue, pain at injection site, gastrointestinal symptoms, and subjective fever. All reported symptoms were of mild (81% adolescents, 82% children) to moderate (19% adolescents, 18% children) intensity (Table 2). As in adults, a general reduction in leukocyte counts was observed in adolescents and children within the first 2 days post-injection; leukocytes gradually restored to baseline values by day 28. An increase in monocyte and lymphocyte counts was observed between days 2 and 7, with lymphocytes rapidly restoring to baseline values by day 7 (S5 Table). No vaccine-related serious or severe adverse events occurred. One child was hospitalised for malaria.

rVSVΔG-ZEBOV-GP viraemia and shedding

Compared to adults vaccinated with 2 × 107 PFU, rVSVΔG-ZEBOV-GP RNA copy numbers in both adolescents and children were significantly higher at 1,592 (IQR 1,019–2,704) and 1,109 (IQR 663–1,963), respectively, versus 532 (IQR 373–898) in adults (P = 0.001) at day 2 post-injection (Table 8).
Table 8

Description of viraemia by dose and age.

Time point*AdultsChildren: 2 × 107 PFUAdolescents: 2 × 107 PFUP value
3 × 103 PFU3 × 104 PFU3 × 105 PFU3 × 106 PFU2 × 107 PFU
NMedian copy number (IQR)NMedian copy number (IQR)NMedian copy number (IQR)NMedian copy number (IQR)NMedian copy number (IQR)NMedian copy number (IQR)NMedian copy number (IQR)
D050 (0–0)60 (0–0)190 (0–0)350 (0–0)160 (0–0)200 (0–0)200 (0–0)0.2
D160 (0–0)80 (0–0)183 (0–13)33228 (150–481)16334 (301–1,001)4731 (507–2,142)19655 (412–912)0.5
D250 (0–0)61 (0–12)194 (0–30)35793 (401–1,286)16532 (373–898)201,109 (663–1,963)191,592 (1,019–2,704)0.001
D750 (0–0)64 (2–51)121 (0–6)327 (0–22)164 (0–29)190 (0–17)170 (0–1)0.1

All viraemia values expressed as median (IQR). P values < 0.05 are given in bold.

*Time point in day(s) since vaccination.

†Kruskal Wallis test. P < 0.05 indicates a significant statistical difference in viraemia values between the 3 groups (adults, children, and adolescents) at each time point at the 2 × 107 PFU dose.

IQR, interquartile range; PFU, plaque-forming units.

All viraemia values expressed as median (IQR). P values < 0.05 are given in bold. *Time point in day(s) since vaccination. †Kruskal Wallis test. P < 0.05 indicates a significant statistical difference in viraemia values between the 3 groups (adults, children, and adolescents) at each time point at the 2 × 107 PFU dose. IQR, interquartile range; PFU, plaque-forming units. For viral shedding, there was a low percentage of positive samples at day 2, albeit below the level of quantification. At day 7, there was 1 child and 1 adolescent who had quantifiable RNA in urine. Saliva investigations showed that 42% and 30%, respectively, of adolescents and children had detectable RNA, corresponding with peak viraemia at day 2. At day 7, a considerably higher proportion of adolescents and children, 78% and 35% respectively, had RNA-positive saliva, with most samples being quantifiable (Figs 2 and S2; S13–S15 Tables).
Fig 2

Viral load in saliva for children and adolescents.

rVSVΔG-ZEBOV-GP (rVSV) RNA copy numbers in saliva presented as log10 rVSV RNA copies/ml from day 2 and 7 (d2 and d7) post-injection in adolescents and children vaccinated with 2 × 107 PFU. The broken line denotes the limit of quantitation, and the dotted line denotes the limit of detection. About 67% (12/18) and 30% (6/20) adolescents and children, respectively, had samples above the limit of quantification at day 7. *P < 0.05; **P < 0.01.PFU, plaque-forming units.

Viral load in saliva for children and adolescents.

rVSVΔG-ZEBOV-GP (rVSV) RNA copy numbers in saliva presented as log10 rVSV RNA copies/ml from day 2 and 7 (d2 and d7) post-injection in adolescents and children vaccinated with 2 × 107 PFU. The broken line denotes the limit of quantitation, and the dotted line denotes the limit of detection. About 67% (12/18) and 30% (6/20) adolescents and children, respectively, had samples above the limit of quantification at day 7. *P < 0.05; **P < 0.01.PFU, plaque-forming units.

Immunogenicity

In all, 90% and 100% of children and adolescents, respectively, receiving 2 × 107 PFU had ZEBOV-GP-specific antibodies at day 28. Antibody titres were similar between adolescents, adults, and children using GP ELISA regardless of baseline antibody status (Figs 3, 4, S3 and S4).
Fig 3

Glycoprotein antibody distribution by age group: Comparison of distribution of ZEBOV-GP IgG antibodies (AEU/ml) measured by USAMRIID ZEBOV-GP ELISA for dose 2 × 107 PFU administered to children, adolescents, and adults from day 0, 28, 56, 84, and 180.

Data were not available for children and adolescents at D84. P < 0.05 indicates a statistical difference in ZEBOV-GP IgG between children, adolescents, and adults. AEU, arbitrary enzyme-linked immunosorbent assay units; ELISA, enzyme-linked immunosorbent assay; GP, glycoprotein; PFU, plaque-forming units; USAMRIID, US Army Medical Research Institute of Infectious Diseases; ZEBOV, Zaire Ebola virus.

Fig 4

Antibody responses to whole-virion ELISA (AEU/ml) by age group: Comparison of geometric mean concentration of IgG antibodies for children, adolescents, and adults vaccinated with the 2 × 107 PFU dose at day 0, 28, and 56.

P < 0.05 indicates a statistical difference in antibody concentrations between age groups at the measured time points. AEU, arbitrary enzyme-linked immunosorbent assay units; ELISA, enzyme-linked immunosorbent assay; PFU, plaque-forming units; ZEBOV, Zaire Ebola virus.

Glycoprotein antibody distribution by age group: Comparison of distribution of ZEBOV-GP IgG antibodies (AEU/ml) measured by USAMRIID ZEBOV-GP ELISA for dose 2 × 107 PFU administered to children, adolescents, and adults from day 0, 28, 56, 84, and 180.

Data were not available for children and adolescents at D84. P < 0.05 indicates a statistical difference in ZEBOV-GP IgG between children, adolescents, and adults. AEU, arbitrary enzyme-linked immunosorbent assay units; ELISA, enzyme-linked immunosorbent assay; GP, glycoprotein; PFU, plaque-forming units; USAMRIID, US Army Medical Research Institute of Infectious Diseases; ZEBOV, Zaire Ebola virus.

Antibody responses to whole-virion ELISA (AEU/ml) by age group: Comparison of geometric mean concentration of IgG antibodies for children, adolescents, and adults vaccinated with the 2 × 107 PFU dose at day 0, 28, and 56.

P < 0.05 indicates a statistical difference in antibody concentrations between age groups at the measured time points. AEU, arbitrary enzyme-linked immunosorbent assay units; ELISA, enzyme-linked immunosorbent assay; PFU, plaque-forming units; ZEBOV, Zaire Ebola virus. By day 28, 70% and 60% of adolescents and children, respectively, were seropositive with whole-virion ELISA, compared to 81% of adults injected with 2 × 107 PFU. Using a more sensitive GP ELISA, we obtained higher seropositivity rates, 100%, 100%, and 90% for adults, adolescents, and children, respectively, at day 28. We observed a ≥4-fold increase in ZEBOV-GP-specific antibody titres in about 90%–100% of adults, adolescents, and children consistently from day 28 to 180 post-injection. However, ZEBOV-GP-specific antibodies increased up to day 180 in children and adolescents (Table 9), while in adults, it peaked at day 56, and there was a decline until day 180 (Tables 3 and 5).
Table 9

Geometric mean titres, seropositivity rates, and proportions of seroresponders to rVSVΔG-ZEBOV-GP measured by ZEBOV-GP ELISA in children.

Cohort (2 × 107 PFU)Time point*NGMT (95% CI)Seropositivity (>200 AEU/ml), N (percent)Seroresponse (≥4×), N (percent)P value
Change in GMTChange in seropositivitySeropositivity and seroresponse
ChildrenD01515 (7–35)0 (0)0 (0)
D28201,620 (806–3,259)18 (90)19 (95)<0.001<0.010.1
D56201,599 (921–2,777)18 (90)20 (100)<0.001<0.011
D180202,069 (1,005–4,258)18 (90)18 (90)<0.001<0.01<0.01
AdolescentsD01512 (5–28)1 (7)0 (0)
D28151,427 (1,024–1,989)15 (100)15 (100)0.0010.0021
D56161,744 (1,264–2,407)16 (100)16 (100)<0.001<0.0011
D180172,541 (1,317–4,906)17 (100)17 (100)<0.001<0.0011

Results are presented as GMTs with 95% confidence intervals. Seropositivity is defined by geometric mean concentration > 200 AEU/ml. Seroresponse is defined by a ≥4-fold rise in GMT. P values < 0.05 are given in bold.

*Time point in day(s) since vaccination.

†Wilcoxon’s test for paired data. P < 0.05 indicates a statistical difference in antibody titre between day 0 and other days.

‡McNemar’s test. P < 0.05 indicates a statistical difference in seropositivity rate between day 0 and other days.

ΩFisher’s test. P < 0.05 indicates a statistical association between seropositivity and seroresponse for each time point.

AEU, arbitrary enzyme-linked immunosorbent assay units; ELISA, enzyme-linked immunosorbent assay; GMT, geometric mean titre; GP, glycoprotein; PFU, plaque-forming units; ZEBOV, Zaire Ebola virus.

Results are presented as GMTs with 95% confidence intervals. Seropositivity is defined by geometric mean concentration > 200 AEU/ml. Seroresponse is defined by a ≥4-fold rise in GMT. P values < 0.05 are given in bold. *Time point in day(s) since vaccination. †Wilcoxon’s test for paired data. P < 0.05 indicates a statistical difference in antibody titre between day 0 and other days. ‡McNemar’s test. P < 0.05 indicates a statistical difference in seropositivity rate between day 0 and other days. ΩFisher’s test. P < 0.05 indicates a statistical association between seropositivity and seroresponse for each time point. AEU, arbitrary enzyme-linked immunosorbent assay units; ELISA, enzyme-linked immunosorbent assay; GMT, geometric mean titre; GP, glycoprotein; PFU, plaque-forming units; ZEBOV, Zaire Ebola virus. Lower proportions of adults, adolescents, and children had a ≥4-fold increase in ZEBOV antibodies with whole-virion ELISA. Considering a ≥2-fold increase for this less sensitive ELISA, the yielded proportions were still much lower than those seen with GP ELISA. However, the proportion of adolescents and children with a ≥2- or ≥4-fold increase in ZEBOV antibodies increased from day 28 to 56, in contrast to the lack of difference between these time points in adults (Tables 5, 6 and S6). Thirteen percent of the children, but none of the adolescents, were seropositive for ZEBOV antibodies at baseline. None of the children and 7% of the adolescents were seropositive for ZEBOV-GP antibodies at baseline. As in adults, children with ZEBOV antibodies at baseline had higher GMTs at days 28 and 56 compared to those without baseline antibodies (Tables 6 and S7). Against VSV pseudovirions, about 73% of children and adolescents elicited Nabs, with higher GMTs occurring at day 56 compared to day 28. In all, 95% and 80% of children and adolescents, respectively, had ZEBOV Nabs at day 28. Overall, children produced significantly higher GMTs of Nabs against ZEBOV particles (20 [95% CI: 13–32] compared to adolescents and adults, 10 [95% CI: 8–14] and 10 [95% CI: 6–14], respectively, P = 0.04) (S10–S12 Tables).

Discussion

Although the 2014–2016 EVD emergency in western Africa has ended, the increasing mobility of people between remote and urban areas and the weak health systems in Ebolavirus endemic countries suggest that a future outbreak could reassert itself as a major international threat [17,18]. Risks include increased human-to-human secondary transmission as in the recent epidemic [19] as well as continuing transmission after recovery. Halting transmission by vaccination will be key in curbing future outbreaks [20]. The rVSVΔG-ZEBOV-GP and ChAd3-ZEBOV vaccine candidates were selected by WHO in August 2014 for fast track clinical evaluation [6]. As part of these efforts, we examined a range of doses for rVSVΔG-ZEBOV-GP in adults as well as safety and immunogenicity in children. As reported earlier, rVSVΔG-ZEBOV-GP doses of 3 × 105 and 3 × 106 PFU were well tolerated by 39 Lambaréné participants until day 28 and were safe up to 6 months [9]. Comparable to studies in Guinea [21] and US adults [7], transient cases of arthralgia were reported after vaccination [9,21,22], but no case of arthritis. In Kilifi, Kenya, there were 2 self-limiting, low-severity, and short-duration cases of arthritis [9,23]. This contrasts with a higher frequency of vaccine-induced arthritis (24%), dermatitis (9.8%), and vasculitis (2%) in Geneva [9,10,24] and more recently in Canada, the US, and Spain [25]. There may be similarities between rVSVΔG-ZEBOV-GP vaccine and rubella vaccine, which also causes transient arthritides in some populations [26-28]. Ongoing studies are investigating the potential mechanisms by which rVSVΔG-ZEBOV-GP vaccine might disseminate into peripheral tissues and induce arthritides in specific hosts. The magnitude of innate immune responses to rVSVΔG-ZEBOV-GP vaccine correlated with the peak of rVSV RNA at day 1 in vaccinees of both Geneva and Lambaréné cohorts [29]. Importantly, high-dose vaccinees who experienced arthritis in Geneva had a significantly lower magnitude of early immune response compared to high-dose vaccinees who did not experience arthritis. These findings suggest that early and appropriate (in nature and magnitude) innate immune responses play a key role in limiting viral replication and dissemination to tissues and thus prevent the risk of arthritis. With lower vaccine dose (3 × 105 PFU), the strength of early innate immune responses was similar in cases both with and without arthritis. Thus, rVSV-ZEBOV-induced arthritis may occur through mechanisms related to either vaccine dose or underlying factors that influence immune responses in vaccinees [29]. We observed higher and persistent viraemia in children and adolescents as well as shedding in saliva and urine, in contrast to the very low proportions or no shedding previously reported in the saliva of American and European adults vaccinated with 3 × 106 to 5 × 107 PFU [7,9,10]. The shedding in saliva did not correlate with oral symptoms. Although no alarming symptoms have been detected so far, our finding suggests that a vaccine dose of 2 × 107 PFU exposed the paediatric population to prolonged or uncontrolled viraemia, with potential to disseminate to peripheral tissues. Specific studies are needed to elucidate the underlying mechanisms prolonging viraemia and causing shedding, such as differences in innate responses to vaccine between adults and younger participants. It is also necessary to assess any potential dissemination of rVSV-ZEBOV among household members of vaccinated children. We observed dose-dependent antibody responses to the rVSVΔG-ZEBOV-GP vaccine. A very low dose (≤3 × 103 PFU) did not generate antibodies measured with either whole-virion or ZEBOV-GP-specific ELISA. In all individuals vaccinated with 3 × 104, 3 × 105, 3 × 106, and 2 × 107 PFU, the vaccine induced significant increases in ZEBOV-GP-specific antibodies measured by ZEBOV-GP ELISA alone for 3 × 104 PFU and by both whole-virion and GP ELISAs for the other vaccine doses. The highest GMTs were observed with 2 × 107 PFU irrespective of the ELISA method used. As previously reported [9,11,12], our participants harboured naturally acquired antibodies against ZEBOV, or possibly related viruses. Western blot analysis of sub-samples showed that these antibodies were directed more often against nucleocapsid and matrix proteins of ZEBOV and not against GP. Nonetheless, 11% of our adults had ZEBOV-GP-specific antibodies before vaccination using the GP-specific ELISA. Individuals with baseline antibodies developed higher antibody titres with a dose as low as 3 × 104 PFU compared to those without. The vaccine may have elicited higher titres of antibodies in the presence of natural GP-specific antibodies but also in the presence of antibodies directed against other viral components including nucleocapsid and matrix proteins (detected in baseline sera of some study participants) [9]. In adults, vaccine-induced antibodies peaked at day 56 and declined slowly by day 180. In children and adolescents, who showed high viraemia at day 2 and shed the vaccine until day 7, antibody titres increased until day 180. The kinetics of antibodies after vaccination may be affected by the specificity of pre-existing antibodies, and persistent vaccine replication may enhance immunogenicity. Also, the highest titres of Nabs against Ebola virus, which paralleled those against VSV pseudovirions, were generated at day 28 post-injection, regardless of baseline seropositivity. The relative roles of neutralising, GP, and non-GP antibodies in protection against EVD remain undefined, so it is difficult to draw conclusions on the clinical significance of correlations between GP-binding and neutralising antibodies produced after vaccinations. The vaccine dose of 2 × 107 PFU showed the optimal safety versus immunogenicity balance in our adult cohorts as well as in the Geneva and Hamburg cohorts [29,30]. These findings support the choice to use this dose in the context of outbreaks [8]. However, our data cannot explain the protection induced by the vaccine within 10 days observed in a phase III trial in Guinea [8] as the seroconversion rates and antibody titres were very weak before day 28 irrespective of the vaccine dose. Innate immune components induced immediately after vaccination may have played an important role in early protection. A recent study demonstrated the direct influence of innate immune responses on this vaccine’s safety and immunogenicity [29], a finding which supports the interest in assessing the efficacy of this vaccine beyond Zaire ebolavirus spp. as innate mechanisms can be cross-reactive. Lower doses could be considered in vaccination strategies for children and individuals with impaired innate immune responses to control early rVSV replication. The dose of 3 × 105 PFU generated significantly fewer rVSV RNA copies and shorter rVSV replication cycles but high antibody titres, so is of interest. As an incidental finding in our area, where Ebola virus transmission is endemic, a proportion of participants had antibodies directed against the whole-virus or GP-specific antigen before vaccination [11,12,31]. In those participants, a vaccine dose as low as 3 × 104 PFU induced high antibody titres, suggesting lower vaccine doses should be considered in boosting strategies. There are some limitations of our observations. For example, we cannot relate viral shedding in saliva with the oral symptoms reported by adolescents and children, suggesting that further studies are needed to evaluate this finding. We did not stratify participants based on antibody status at enrolment; future studies in Ebola virus endemic areas where such stratification is inherent in the design will provide insights into the relationships between naturally acquired antibodies and vaccine-induced immune responses and safety. We enrolled very few women across cohorts, leading to imbalances in the male/female ratio in our trial, which may reflect the general reluctance of women to enrol in phase I studies. Our study confirms the acceptable safety and immunogenicity profile of the 2 × 107 PFU dose in adults. However, considering the persistent replication of the rVSVΔGP-ZEBOV-GP vaccine in children and adolescents, further studies investigating lower doses in this population are warranted. In addition, lower vaccine doses should be considered when boosting individuals with pre-existing antibodies.

Study vaccine reconstitution.

(DOCX) Click here for additional data file.

Viral load and viraemia in children, adolescents, and adults.

(DOCX) Click here for additional data file.

ZEBOV-GP-specific antibodies by age group in individuals without baseline antibodies.

(DOCX) Click here for additional data file.

ZEBOV antibodies measured by whole-virion ELISA by age group in individuals without baseline antibodies.

(DOCX) Click here for additional data file.

Reactogenicity to rVSV-ZEBOV-GP vaccine until day 28.

(DOCX) Click here for additional data file.

Reactogenicity to rVSV-ZEBOV-GP vaccine until day 28 in vaccinees with baseline ZEBOV-specific antibodies.

(DOCX) Click here for additional data file.

Reactogenicity to rVSV-ZEBOV-GP vaccine until day 28 in vaccinees without baseline ZEBOV-specific antibodies.

(DOCX) Click here for additional data file.

Frequency of symptoms after day 28 in adults.

(DOCX) Click here for additional data file.

Haematology and biochemistry parameters.

(DOCX) Click here for additional data file.

ZEBOV antibodies in geometric mean titres measured by whole-virion ELISA in children and adolescents.

(DOCX) Click here for additional data file.

ZEBOV antibodies by baseline status in children measured by whole-virion ELISA.

(DOCX) Click here for additional data file.

Neutralising antibodies to infectious ZEBOV isolate in adults.

(DOCX) Click here for additional data file.

Neutralising antibodies to infectious ZEBOV isolate classified by baseline ZEBOV antibody status in adults.

(DOCX) Click here for additional data file.

Neutralising antibodies to ZEBOV in children and adolescents.

(DOCX) Click here for additional data file.

Neutralising antibodies to VSV peudovirions measured by PsVNA50 in children and adolescents.

(DOCX) Click here for additional data file.

Comparison of antibodies in adults, children, and adolescents.

(DOCX) Click here for additional data file.

rVSV RNA shedding and proportion of adolescents and children with detectable and quantifiable viral RNA.

(DOCX) Click here for additional data file.

Viraemia in participants with baseline ZEBOV antibodies.

(DOCX) Click here for additional data file.

Viraemia in participants without baseline ZEBOV antibodies.

(DOCX) Click here for additional data file.

Trial protocol.

(PDF) Click here for additional data file.

CONSORT checklist.

(DOC) Click here for additional data file.

Dose escalation and randomisation.

(DOCX) Click here for additional data file.

Data collection, management, and safety assessment.

(DOCX) Click here for additional data file.
  23 in total

1.  Use of low dose rVSV-ZEBOV: safety issues in a Swiss cohort.

Authors:  Julie E Ledgerwood
Journal:  Lancet Infect Dis       Date:  2015-08-04       Impact factor: 25.071

2.  A Recombinant Vesicular Stomatitis Virus Ebola Vaccine.

Authors:  Jason A Regules; John H Beigel; Kristopher M Paolino; Jocelyn Voell; Amy R Castellano; Zonghui Hu; Paula Muñoz; James E Moon; Richard C Ruck; Jason W Bennett; Patrick S Twomey; Ramiro L Gutiérrez; Shon A Remich; Holly R Hack; Meagan L Wisniewski; Matthew D Josleyn; Steven A Kwilas; Nicole Van Deusen; Olivier Tshiani Mbaya; Yan Zhou; Daphne A Stanley; Wang Jing; Kirsten S Smith; Meng Shi; Julie E Ledgerwood; Barney S Graham; Nancy J Sullivan; Linda L Jagodzinski; Sheila A Peel; Judie B Alimonti; Jay W Hooper; Peter M Silvera; Brian K Martin; Thomas P Monath; W Jay Ramsey; Charles J Link; H Clifford Lane; Nelson L Michael; Richard T Davey; Stephen J Thomas
Journal:  N Engl J Med       Date:  2015-04-01       Impact factor: 91.245

3.  Randomised double-blind placebo-controlled study on adverse effects of rubella immunisation in seronegative women.

Authors:  A J Tingle; L A Mitchell; M Grace; P Middleton; R Mathias; L MacWilliam; A Chalmers
Journal:  Lancet       Date:  1997-05-03       Impact factor: 79.321

4.  High prevalence of both humoral and cellular immunity to Zaire ebolavirus among rural populations in Gabon.

Authors:  Pierre Becquart; Nadia Wauquier; Tanel Mahlakõiv; Dieudonné Nkoghe; Cindy Padilla; Marc Souris; Benjamin Ollomo; Jean-Paul Gonzalez; Xavier De Lamballerie; Mirdad Kazanji; Eric M Leroy
Journal:  PLoS One       Date:  2010-02-09       Impact factor: 3.240

5.  Efficacy and effectiveness of an rVSV-vectored vaccine expressing Ebola surface glycoprotein: interim results from the Guinea ring vaccination cluster-randomised trial.

Authors:  Ana Maria Henao-Restrepo; Ira M Longini; Matthias Egger; Natalie E Dean; W John Edmunds; Anton Camacho; Miles W Carroll; Moussa Doumbia; Bertrand Draguez; Sophie Duraffour; Godwin Enwere; Rebecca Grais; Stephan Gunther; Stefanie Hossmann; Mandy Kader Kondé; Souleymane Kone; Eeva Kuisma; Myron M Levine; Sema Mandal; Gunnstein Norheim; Ximena Riveros; Aboubacar Soumah; Sven Trelle; Andrea S Vicari; Conall H Watson; Sakoba Kéïta; Marie Paule Kieny; John-Arne Røttingen
Journal:  Lancet       Date:  2015-08-03       Impact factor: 79.321

6.  Efficacy and effectiveness of an rVSV-vectored vaccine in preventing Ebola virus disease: final results from the Guinea ring vaccination, open-label, cluster-randomised trial (Ebola Ça Suffit!).

Authors:  Ana Maria Henao-Restrepo; Anton Camacho; Ira M Longini; Conall H Watson; W John Edmunds; Matthias Egger; Miles W Carroll; Natalie E Dean; Ibrahima Diatta; Moussa Doumbia; Bertrand Draguez; Sophie Duraffour; Godwin Enwere; Rebecca Grais; Stephan Gunther; Pierre-Stéphane Gsell; Stefanie Hossmann; Sara Viksmoen Watle; Mandy Kader Kondé; Sakoba Kéïta; Souleymane Kone; Eewa Kuisma; Myron M Levine; Sema Mandal; Thomas Mauget; Gunnstein Norheim; Ximena Riveros; Aboubacar Soumah; Sven Trelle; Andrea S Vicari; John-Arne Røttingen; Marie-Paule Kieny
Journal:  Lancet       Date:  2016-12-23       Impact factor: 79.321

7.  Mapping the zoonotic niche of Ebola virus disease in Africa.

Authors:  David M Pigott; Nick Golding; Adrian Mylne; Zhi Huang; Andrew J Henry; Daniel J Weiss; Oliver J Brady; Moritz U G Kraemer; David L Smith; Catherine L Moyes; Samir Bhatt; Peter W Gething; Peter W Horby; Isaac I Bogoch; John S Brownstein; Sumiko R Mekaru; Andrew J Tatem; Kamran Khan; Simon I Hay
Journal:  Elife       Date:  2014-09-08       Impact factor: 8.140

8.  Use of ChAd3-EBO-Z Ebola virus vaccine in Malian and US adults, and boosting of Malian adults with MVA-BN-Filo: a phase 1, single-blind, randomised trial, a phase 1b, open-label and double-blind, dose-escalation trial, and a nested, randomised, double-blind, placebo-controlled trial.

Authors:  Milagritos D Tapia; Samba O Sow; Kirsten E Lyke; Fadima Cheick Haidara; Fatoumata Diallo; Moussa Doumbia; Awa Traore; Flanon Coulibaly; Mamoudou Kodio; Uma Onwuchekwa; Marcelo B Sztein; Rezwanul Wahid; James D Campbell; Marie-Paule Kieny; Vasee Moorthy; Egeruan B Imoukhuede; Tommy Rampling; Francois Roman; Iris De Ryck; Abbie R Bellamy; Len Dally; Olivier Tshiani Mbaya; Aurélie Ploquin; Yan Zhou; Daphne A Stanley; Robert Bailer; Richard A Koup; Mario Roederer; Julie Ledgerwood; Adrian V S Hill; W Ripley Ballou; Nancy Sullivan; Barney Graham; Myron M Levine
Journal:  Lancet Infect Dis       Date:  2015-11-04       Impact factor: 25.071

9.  Dose-dependent T-cell Dynamics and Cytokine Cascade Following rVSV-ZEBOV Immunization.

Authors:  Christine Dahlke; Rahel Kasonta; Sebastian Lunemann; Verena Krähling; Madeleine E Zinser; Nadine Biedenkopf; Sarah K Fehling; My L Ly; Anne Rechtien; Hans C Stubbe; Flaminia Olearo; Saskia Borregaard; Alen Jambrecina; Felix Stahl; Thomas Strecker; Markus Eickmann; Marc Lütgehetmann; Michael Spohn; Stefan Schmiedel; Ansgar W Lohse; Stephan Becker; Marylyn M Addo
Journal:  EBioMedicine       Date:  2017-04-05       Impact factor: 8.143

10.  Will Ebola change the game? Ten essential reforms before the next pandemic. The report of the Harvard-LSHTM Independent Panel on the Global Response to Ebola.

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Journal:  Lancet       Date:  2015-11-23       Impact factor: 79.321
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1.  The Sierra Leone Trial to Introduce a Vaccine Against Ebola: An Evaluation of rVSV∆G-ZEBOV-GP Vaccine Tolerability and Safety During the West Africa Ebola Outbreak.

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Journal:  J Infect Dis       Date:  2018-05-18       Impact factor: 5.226

2.  Pseudovirus rVSVΔG-ZEBOV-GP Infects Neurons in Retina and CNS, Causing Apoptosis and Neurodegeneration in Neonatal Mice.

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Journal:  Cell Rep       Date:  2019-02-12       Impact factor: 9.423

3.  Description of vaccine clinical trials in Africa: a narrative review.

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Journal:  Hum Vaccin Immunother       Date:  2019-12-12       Impact factor: 3.452

4.  Pre-clinical development of a vaccine against Lassa fever.

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Journal:  Can Commun Dis Rep       Date:  2018-06-07

Review 5.  Therapeutic vaccination strategies against EBOV by rVSV-EBOV-GP: the role of innate immunity.

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Journal:  Curr Opin Virol       Date:  2021-11-05       Impact factor: 7.090

6.  Thermostable Ebola virus vaccine formulations lyophilized in the presence of aluminum hydroxide.

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Journal:  Eur J Pharm Biopharm       Date:  2019-01-28       Impact factor: 5.571

7.  Baseline Asymptomatic Malaria Infection and Immunogenicity of Recombinant Vesicular Stomatitis Virus-Zaire Ebola Virus Envelope Glycoprotein.

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Review 8.  The Status and Prospects of Epstein-Barr Virus Prophylactic Vaccine Development.

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