| Literature DB >> 33529172 |
Kenta Matsuda1, Stephen A Migueles1, Jinghe Huang1, Lyuba Bolkhovitinov1, Sarah Stuccio1, Trevor Griesman1, Alyssa A Pullano1, Byong H Kang1, Elise Ishida1, Matthew Zimmerman1, Neena Kashyap1, Kelly M Martins1, Daniel Stadlbauer2, Jessica Pederson1, Andy Patamawenu1, Nathaniel Wright1, Tulley Shofner1, Sean Evans1, C Jason Liang3, Julián Candia4, Angelique Biancotto4, Giovanna Fantoni4, April Poole1, Jon Smith5, Jeff Alexander5, Marc Gurwith5, Florian Krammer2, Mark Connors1.
Abstract
BACKGROUNDTo understand the features of a replicating vaccine that might drive potent and durable immune responses to transgene-encoded antigens, we tested a replication-competent adenovirus type 4 encoding influenza virus H5 HA (Ad4-H5-Vtn) administered as an oral capsule or via tonsillar swab or nasal spray.METHODSViral shedding from the nose, mouth, and rectum was measured by PCR and culturing. H5-specific IgG and IgA antibodies were measured by bead array binding assays. Serum antibodies were measured by a pseudovirus entry inhibition, microneutralization, and HA inhibition assays.RESULTSAd4-H5-Vtn DNA was shed from most upper respiratory tract-immunized (URT-immunized) volunteers for 2 to 4 weeks, but cultured from only 60% of participants, with a median duration of 1 day. Ad4-H5-Vtn vaccination induced increases in H5-specific CD4+ and CD8+ T cells in the peripheral blood as well as increases in IgG and IgA in nasal, cervical, and rectal secretions. URT immunizations induced high levels of serum neutralizing antibodies (NAbs) against H5 that remained stable out to week 26. The duration of viral shedding correlated with the magnitude of the NAb response at week 26. Adverse events (AEs) were mild, and peak NAb titers were associated with overall AE frequency and duration. Serum NAb titers could be boosted to very high levels 2 to 5 years after Ad4-H5-Vtn vaccination with recombinant H5 or inactivated split H5N1 vaccine.CONCLUSIONReplicating Ad4 delivered to the URT caused prolonged exposure to antigen, drove durable systemic and mucosal immunity, and proved to be a promising platform for the induction of immunity against viral surface glycoprotein targets.TRIAL REGISTRATIONClinicalTrials.gov NCT01443936 and NCT01806909.FUNDINGIntramural and Extramural Research Programs of the NIAID, NIH (U19 AI109946) and the Centers of Excellence for Influenza Research and Surveillance (CEIRS), NIAID, NIH (contract HHSN272201400008C).Entities:
Keywords: Adaptive immunity; Beta cells; Immunology; Influenza; Vaccines
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Year: 2021 PMID: 33529172 PMCID: PMC7919717 DOI: 10.1172/JCI140794
Source DB: PubMed Journal: J Clin Invest ISSN: 0021-9738 Impact factor: 14.808