Nonhuman primate to human immunobridging to infer the protective effect of an Ebola virus vaccine candidate

Author:

Roozendaal RamonORCID,Hendriks Jenny,van Effelterre Thierry,Spiessens Bart,Dekking Liesbeth,Solforosi Laura,Czapska-Casey Dominika,Bockstal Viki,Stoop Jeroen,Splinter Daniel,Janssen Sarah,Baelen Ben van,Verbruggen Nadia,Serroyen Jan,Dekeyster Eline,Volkmann Ariane,Wollmann Yvonne,Carrion Ricardo,Giavedoni Luis D.,Robinson Cynthia,Leyssen Maarten,Douoguih Macaya,Luhn Kerstin,Pau Maria Grazia,Sadoff Jerry,Vandebosch An,Schuitemaker HannekeORCID,Zahn RolandORCID,Callendret Benoit

Abstract

AbstractIt has been proven challenging to conduct traditional efficacy trials for Ebola virus (EBOV) vaccines. In the absence of efficacy data, immunobridging is an approach to infer the likelihood of a vaccine protective effect, by translating vaccine immunogenicity in humans to a protective effect, using the relationship between vaccine immunogenicity and the desired outcome in a suitable animal model. We here propose to infer the protective effect of the Ad26.ZEBOV, MVA-BN-Filo vaccine regimen with an 8-week interval in humans by immunobridging. Immunogenicity and protective efficacy data were obtained for Ad26.ZEBOV and MVA-BN-Filo vaccine regimens using a fully lethal EBOV Kikwit challenge model in cynomolgus monkeys (nonhuman primates [NHP]). The association between EBOV neutralizing antibodies, glycoprotein (GP)-binding antibodies, and GP-reactive T cells and survival in NHP was assessed by logistic regression analysis. Binding antibodies against the EBOV surface GP were identified as the immune parameter with the strongest correlation to survival post EBOV challenge, and used to infer the predicted protective effect of the vaccine in humans using published data from phase I studies. The human vaccine-elicited EBOV GP-binding antibody levels are in a range associated with significant protection against mortality in NHP. Based on this immunobridging analysis, the EBOV GP-specific-binding antibody levels elicited by the Ad26.ZEBOV, MVA-BN-Filo vaccine regimen in humans will likely provide protection against EBOV disease.

Publisher

Springer Science and Business Media LLC

Subject

Pharmacology (medical),Infectious Diseases,Pharmacology,Immunology

Reference53 articles.

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