Intranasal M2SR (M2-Deficient Single Replication) H3N2 Influenza Vaccine Provides Enhanced Mucosal and Serum Antibodies in Adults

Author:

Eiden Joseph1,Fierro Carlos2,Schwartz Howard3,Adams Mark4,Ellis Kimberly J5,Aitchison Roger6,Herber Renee1,Hatta Yasuko1,Marshall David1,Moser Michael J1,Belshe Robert7,Greenberg Harry8,Coelingh Kathleen9,Kawaoka Yoshihiro10,Neumann Gabriele10,Bilsel Pamuk1

Affiliation:

1. FluGen, Inc , Madison, Wisconsin , USA

2. Johnson County Clin-Trials , Lenexa, Kansas , USA

3. Research Centers of America , Hollywood, Florida , USA

4. Alliance for Multispecialty Research , Lexington, Kentucky , USA

5. Alliance for Multispecialty Research , Norfolk, Virginia , USA

6. North Rim Consulting , Longmont, Colorado , USA

7. Saint Louis University , St Louis, Missouri , USA

8. Stanford University , Stanford, California , USA

9. St Helena , California , USA

10. Influenza Research Institute, University of Wisconsin , Madison, Wisconsin , USA

Abstract

Abstract Background We previously demonstrated that an intranasal dose of 108 50% tissue culture infectious dose (TCID50) M2-deficient single replication (M2SR) influenza vaccine protected against highly drifted H3N2 influenza challenge in a subset of subjects who demonstrated ≥2-fold increase in microneutralization (MN) antibodies to Belgium2015 (the challenge strain) after vaccination. Here, we describe a phase 1b, observer-blinded, dose-escalation study demonstrating an increased proportion of responders with this signal of immune protection. Methods Serosusceptible subjects aged 18–49 years were randomized to receive 2 doses (108–109 TCID50) of M2SR or placebo administered 28 days apart. Clinical specimens were collected before and after each dose. The primary objective was to demonstrate safety of M2SR vaccines. Results The vaccine was well tolerated at all dose levels. Against Belgium2015, ≥ 2-fold increases in MN antibodies were noted among 40% (95% confidence interval [CI], 24.9%–56.7%) of subjects following a single 108 TCID50 M2SR dose and among 80.6% (95% CI, 61.4%–92.3%) after 109 dose (P < .001). A single 109 TCID50 dose of M2SR generated ≥4-fold hemagglutination inhibition antibody seroconversion against the vaccine strain in 71% (95% CI, 52.0%–85.8%) of recipients. Mucosal and cellular immune responses were also induced. Conclusions These results indicate that M2SR may provide substantial protection against infection with highly drifted strains of H3N2 influenza. Clinical Trials Registration NCT03999554.

Funder

Office of the Assistant Secretary of Defense for Health Affairs

Publisher

Oxford University Press (OUP)

Subject

Infectious Diseases,Immunology and Allergy

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