Chimeric Hemagglutinin-Based Influenza Virus Vaccines Induce Protective Stalk-Specific Humoral Immunity and Cellular Responses in Mice

The high variation of the influenza virus hemagglutinin (HA), particularly of its immunodominant head epitopes, makes it necessary to reformulate seasonal influenza virus vaccines every year. Novel influenza virus vaccines that redirect the immune response toward conserved epitopes of the HA stalk d...

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Published in:ImmunoHorizons Vol. 3; no. 4; pp. 133 - 148
Main Authors: Choi, Angela, Bouzya, Badiaa, Cortés Franco, Klaus-Daniel, Stadlbauer, Daniel, Rajabhathor, Arvind, Rouxel, Ronan N, Mainil, Roland, Van der Wielen, Marie, Palese, Peter, García-Sastre, Adolfo, Innis, Bruce L, Krammer, Florian, Schotsaert, Michael, Mallett, Corey P, Nachbagauer, Raffael
Format: Journal Article
Language:English
Published: United States 01-04-2019
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Summary:The high variation of the influenza virus hemagglutinin (HA), particularly of its immunodominant head epitopes, makes it necessary to reformulate seasonal influenza virus vaccines every year. Novel influenza virus vaccines that redirect the immune response toward conserved epitopes of the HA stalk domain should afford broad and durable protection. Sequential immunization with chimeric HAs (cHAs) that express the same conserved HA stalk and distinct exotic HA heads has been shown to elicit high levels of broadly cross-reactive Abs. In the current mouse immunization studies, we tested this strategy using inactivated split virion cHA influenza virus vaccines (IIV) without adjuvant or adjuvanted with AS01 or AS03 to measure the impact of adjuvant on the Ab response. The vaccines elicited high levels of cross-reactive Abs that showed activity in an Ab-dependent, cell-mediated cytotoxicity reporter assay and were protective in a mouse viral challenge model after serum transfer. In addition, T cell responses to adjuvanted IIV were compared with responses to a cHA-expressing live attenuated influenza virus vaccine (LAIV). A strong but transient induction of Ag-specific T cells was observed in the spleens of mice vaccinated with LAIV. Interestingly, IIV also induced T cells, which were successfully recalled upon viral challenge. Groups that received AS01-adjuvanted IIV or LAIV 4 wk before the challenge showed the lowest level of viral replication (i.e., the highest level of protection). These studies provide evidence that broadly cross-reactive Abs elicited by cHA vaccination demonstrate Fc-mediated activity. In addition, cHA vaccination induced Ag-specific cellular responses that can contribute to protection upon infection.
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Current address: PATH, Washington, DC.
M.V.d.W., P.P., A.G.-S., B.L.I., F.K., M.S., C.P.M., and R.N. were involved in the conception and/or the design of the studies. A.C., B.B., K.-D.C.F., D.S., and A.R., developed protocol(s) for the study and/or acquired the data. A.C., B.B., K.-D.C.F., D.S., A.R., R.N.R., R.M., P.P., A.G.-S., B.L.I., F.K., M.S., C.P.M., and R.N. analyzed and interpreted the results. All authors were involved in drafting the manuscript or revising it critically for important intellectual content. All authors had full access to the data and approved the manuscript before it was submitted by the corresponding author.
ISSN:2573-7732
2573-7732
DOI:10.4049/immunohorizons.1900022