The findings, published in the the New England Journal of Medicine, are based on a study of 1,500 adults that began during the West Africa Ebola outbreak.
"This clinical trial has yielded valuable information that is essential for the continued development of these two Ebola vaccine candidates and also demonstrates that well- designed, ethically sound clinical research can be conducted during an epidemic," said Anthony S Fauci, Director of the US National Institute of Allergy and Infectious Diseases (NIAID).
The trial enrolled men and women ages 18 and older with no reported history of Ebola virus disease at Redemption Hospital in Monrovia.
Three groups of 500 volunteers received one of the vaccine candidates or a placebo (saline injection).
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Participants provided blood samples before vaccination and again at one week, one month, six months and one year post-vaccination. Investigators then tested each of these samples for antibodies to the Ebola virus.
Responses at one week were modest with both vaccines. However, by one month, 71 per cent of cAd3-EBOZ recipients and 84 per cent of rVSV-ZEBOV recipients developed an antibody response compared to 3 per cent of placebo recipients.
Some participants who received the investigational vaccines experienced mild to moderate side effects that resolved, such as headache, muscle pain, feverishness and fatigue.
Overall, researchers did not identify any major safety concerns related to the vaccines. Most of the serious medical issues reported during the trial were due to malaria.
At the beginning of the trial investigators found that four per cent of participants already had a certain threshold of Ebola antibodiesindicative of past Ebola infection - but no known history of Ebola virus disease.
Future studies are needed to determine if this is a chance finding or if it has some significance related to cross-reactive immunity.