TY - JOUR
T1 - Randomized Trial of Vaccines for Zaire Ebola Virus Disease
AU - PREVAC Study Team
AU - Kieh, Mark
AU - Richert, Laura
AU - Beavogui, Abdoul H.
AU - Grund, Birgit
AU - Leigh, Bailah
AU - D'Ortenzio, Eric
AU - Doumbia, Seydou
AU - Lhomme, Edouard
AU - Sow, Samba
AU - Vatrinet, Renaud
AU - Roy, Céline
AU - Kennedy, Stephen B.
AU - Faye, Sylvain
AU - Lees, Shelley
AU - Millimouno, Niouma P.
AU - Camara, Alseny M.
AU - Samai, Mohamed
AU - Deen, Gibrilla F.
AU - Doumbia, Moussa
AU - Espérou, Hélène
AU - Pierson, Jerome
AU - Watson-Jones, Deborah
AU - Diallo, Alpha
AU - Wentworth, Deborah
AU - McLean, Chelsea
AU - Simon, Jakub
AU - Wiedemann, Aurélie
AU - Dighero-Kemp, Bonnie
AU - Hensley, Lisa
AU - Lane, H. Clifford
AU - Levy, Yves
AU - Piot, Peter
AU - Greenwood, Brian
AU - Chene, Geneviève
AU - Neaton, James
AU - Yazdanpanah, Yazdan
AU - Ishola, David
N1 - Publisher Copyright:
© 2022 Massachusetts Medical Society.
PY - 2022/12/14
Y1 - 2022/12/14
N2 - Background Questions remain concerning the rapidity of immune responses and the durability and safety of vaccines used to prevent Zaire Ebola virus disease. Methods We conducted two randomized, placebo-controlled trials - one involving adults and one involving children - to evaluate the safety and immune responses of three vaccine regimens against Zaire Ebola virus disease: Ad26.ZEBOV followed by MVA-BN-Filo 56 days later (the Ad26-MVA group), rVSVG-ZEBOV-GP followed by placebo 56 days later (the rVSV group), and rVSVG-ZEBOV-GP followed by rVSVG-ZEBOV-GP 56 days later (the rVSV-booster group). The primary end point was antibody response at 12 months, defined as having both a 12-month antibody concentration of at least 200 enzyme-linked immunosorbent assay units (EU) per milliliter and an increase from baseline in the antibody concentration by at least a factor of 4. Results A total of 1400 adults and 1401 children underwent randomization. Among both adults and children, the incidence of injection-site reactions and symptoms (e.g., feverishness and headache) was higher in the week after receipt of the primary and second or booster vaccinations than after receipt of placebo but not at later time points. These events were largely low-grade. At month 12, a total of 41% of adults (titer, 401 EU per milliliter) and 78% of children (titer, 828 EU per milliliter) had a response in the Ad26-MVA group; 76% (titer, 992 EU per milliliter) and 87% (titer, 1415 EU per milliliter), respectively, had a response in the rVSV group; 81% (titer, 1037 EU per milliliter) and 93% (titer, 1745 EU per milliliter), respectively, had a response in the rVSV-booster group; and 3% (titer, 93 EU per milliliter) and 4% (titer, 67 EU per milliliter), respectively, had a response in the placebo group (P<0.001 for all comparisons of vaccine with placebo). In both adults and children, antibody responses with vaccine differed from those with placebo beginning on day 14.Conclusions No safety concerns were identified in this trial. With all three vaccine regimens, immune responses were seen from day 14 through month 12. (Funded by the National Institutes of Health and others; PREVAC ClinicalTrials.gov number, NCT02876328; EudraCT numbers, 2017-001798-18 and 2017-001798-18/3rd; and Pan African Clinical Trials Registry number, PACTR201712002760250.)
AB - Background Questions remain concerning the rapidity of immune responses and the durability and safety of vaccines used to prevent Zaire Ebola virus disease. Methods We conducted two randomized, placebo-controlled trials - one involving adults and one involving children - to evaluate the safety and immune responses of three vaccine regimens against Zaire Ebola virus disease: Ad26.ZEBOV followed by MVA-BN-Filo 56 days later (the Ad26-MVA group), rVSVG-ZEBOV-GP followed by placebo 56 days later (the rVSV group), and rVSVG-ZEBOV-GP followed by rVSVG-ZEBOV-GP 56 days later (the rVSV-booster group). The primary end point was antibody response at 12 months, defined as having both a 12-month antibody concentration of at least 200 enzyme-linked immunosorbent assay units (EU) per milliliter and an increase from baseline in the antibody concentration by at least a factor of 4. Results A total of 1400 adults and 1401 children underwent randomization. Among both adults and children, the incidence of injection-site reactions and symptoms (e.g., feverishness and headache) was higher in the week after receipt of the primary and second or booster vaccinations than after receipt of placebo but not at later time points. These events were largely low-grade. At month 12, a total of 41% of adults (titer, 401 EU per milliliter) and 78% of children (titer, 828 EU per milliliter) had a response in the Ad26-MVA group; 76% (titer, 992 EU per milliliter) and 87% (titer, 1415 EU per milliliter), respectively, had a response in the rVSV group; 81% (titer, 1037 EU per milliliter) and 93% (titer, 1745 EU per milliliter), respectively, had a response in the rVSV-booster group; and 3% (titer, 93 EU per milliliter) and 4% (titer, 67 EU per milliliter), respectively, had a response in the placebo group (P<0.001 for all comparisons of vaccine with placebo). In both adults and children, antibody responses with vaccine differed from those with placebo beginning on day 14.Conclusions No safety concerns were identified in this trial. With all three vaccine regimens, immune responses were seen from day 14 through month 12. (Funded by the National Institutes of Health and others; PREVAC ClinicalTrials.gov number, NCT02876328; EudraCT numbers, 2017-001798-18 and 2017-001798-18/3rd; and Pan African Clinical Trials Registry number, PACTR201712002760250.)
KW - Global Health
KW - Infectious Disease
KW - Infectious Disease General
KW - Vaccines
KW - Viral Infections
U2 - 10.1056/NEJMoa2200072
DO - 10.1056/NEJMoa2200072
M3 - Article
C2 - 36516078
AN - SCOPUS:85145056550
SN - 0028-4793
VL - 387
SP - 2411
EP - 2424
JO - New England Journal of Medicine
JF - New England Journal of Medicine
IS - 26
ER -
