Longitudinal antibody and T cell responses in Ebola virus disease survivors and contacts: an observational cohort study
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Titre
Longitudinal antibody and T cell responses in Ebola virus disease survivors and contacts: an observational cohort study
Sujet
Description
The 2013–16 Ebola virus disease epidemic in west Africa caused international alarm due to its rapid and extensive spread resulting in a significant death toll and social unrest within the affected region. The large number of cases provided an opportunity to study the long-term kinetics of Zaire ebolavirus-specific immune response of survivors in addition to known contacts of those infected with the virus.
A response to this article was published:
A response to this article was published:
- Etard, Jean-François. "Immunity to Ebola virus: the full picture is being revealed." The Lancet Infectious Diseases.
Date
2020-10-13
Type
Citer ce document
Thom, Ruth, Thomas Tipton, Thomas Strecker, Yper Hall, Joseph Akoi Bore, Piet Maes, Fara Raymond Koundouno, Sarah Katharina Fehling, Verena Krähling, Kimberley Steeds, Anitha Varghese, Graham Bailey, Mary Matheson, Moussa Coné, Balla Moussa Keita, Sekou Kouyate, Amento Richard Ablam, Lies Laenen, Valentijn Vergote, Malcolm Guiver, Joseph Timothy, Barry Atkinson, Lisa Ottowell, Kevin S. Richards, Andrew Bosworth, Stephanie Longet, Jack Mellors, Delphine Pannetier, Sophie Duraffour, César Muñoz-Fontela, Oumou Sow, Lamine Koivogui, Edmund Newman, Stephan Becker, Armand Sprecher, Herve Raoul, Julian Hiscox, Ana Maria Henao-Restrepo, Keita Sakoba, N'Faly Magassouba, Stephan Günther, Mandy Kader Konde, and Miles W. Carroll. 2020. "Longitudinal antibody and T cell responses in Ebola virus disease survivors and contacts: an observational cohort study." The Lancet Infectious Diseases.
Résumé
Summary
Background
The 2013–16 Ebola virus disease epidemic in west Africa caused international alarm due to its rapid and extensive spread resulting in a significant death toll and social unrest within the affected region. The large number of cases provided an opportunity to study the long-term kinetics of Zaire ebolavirus-specific immune response of survivors in addition to known contacts of those infected with the virus.
Methods
In this observational cohort study, we worked with leaders of Ebola virus disease survivor associations in two regions of Guinea, Guéckédou and Coyah, to recruit survivors of Ebola virus disease, contacts from households of individuals known to have had Ebola virus disease, and individuals who were not knowingly associated with infected individuals or had not had Ebola virus disease symptoms to serve as negative controls. We did Zaire ebolavirus glycoprotein-specific T cell analysis on peripheral blood mononuclear cells (PBMCs) on location in Guinea and transported plasma and PBMCs back to Europe for antibody quantification by ELISA, functional neutralising antibody analysis using live Zaire ebolavirus, and T cell phenotype studies. We report on the longitudinal cellular and humoral response among Ebola virus disease survivors and highlight potentially paucisymptomatic infection.
Findings
We recruited 117 survivors of Ebola virus disease, 66 contacts, and 23 negative controls. The mean neutralising antibody titre among the Ebola virus disease survivors 3–14 months after infection was 1/174 (95% CI 1/136—1/223). Individual results varied greatly from 1/10 to more than 1/1000 but were on average ten times greater than that induced after 1 month by single dose Ebola virus vaccines. Following reactivation with glycoprotein peptide, the mean T cell responses among 116 Ebola virus disease survivors as measured by ELISpot was 305 spot-forming units (95% CI 257–353). The dominant CD8+ polyfunctional T cell phenotype, as measured among 53 Ebola virus disease survivors, was interferon γ+, tumour necrosis factor+, interleukin-2–, and the mean response was 0·046% of total CD8+ T cells (95% CI 0·021–0·071). Additionally, both neutralising antibody and T cell responses were detected in six (9%) of 66 Ebola virus disease contacts. We also noted that four (3%) of 117 individuals with Ebola virus disease infections did not have circulating Ebola virus-specific antibodies 3 months after infection.
Interpretation
The continuous high titre of neutralising antibodies and increased T cell response might support the concept of long-term protective immunity in survivors. The existence of antibody and T cell responses in contacts of individuals with Ebola virus disease adds further evidence to the existence of sub-clinical Ebola virus infection.
Funding
US Food & Drug Administration, Horizon 2020 EU EVIDENT, Wellcome, UK Department for International Development.
Accessibilité
Free online on Lancet site.
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