Choice of Adjuvant and Antigen Composition Alters the Immunogenic Profile of a SARS-CoV-2 Subunit Vaccine

Authors

William R Lykins
Jeroen Pollet
Jessica A White
Brian Keegan
Leroy Versteeg
Ulrich Strych
Wen-Hsiang Chen
Raodoh Mohamath
Gabi Ramer-Denisoff
Sierra Reed
Samuel Beaver
Alana Gerhardt
Emily A Voigt
Mark A Tomai
Robert Sitrin
Robert K M Choy
Frederick J Cassels
Peter J Hotez
Maria Elena Bottazzi
Christopher B Fox

Language

English

Publication Date

1-1-2024

Journal

Frontiers in Drug Delivery

DOI

10.3389/fddev.2024.1342518

PMID

40836992

PMCID

PMC12363249

PubMedCentral® Posted Date

2-7-2024

PubMedCentral® Full Text Version

Post-print

Abstract

Introduction: Since their introduction, adjuvanted recombinant subunit vaccines against COVID-19 have played a pivotal role in protecting global populations. Optimizing the immune response's quality, amplitude, and durability to these vaccines depends on the appropriate adjuvant choice and dose in combination with the selected antigen.

Methods: Here, we employed a preclinical mouse model to study the adaptive humoral and cellular immune responses to a SARS-CoV-2 receptor binding domain (RBD) antigen formulated with one of four different immune agonists [GLA, 3M-052, CpG-1826 (CpG), and dmLT], in combination with one of two different immune-stimulating formulations, a stabilized squalene emulsion (SE) or aluminum hydroxide (Alum). Using a weighted desirability index, we established an immunogenicity ranking for each adjuvant in combination with the RBD antigen.

Results: We found that formulations of the RBD with Alum in combination with either 3M-052 or CpG led to at least a 2-log increase in serum IgG production and a 1.3- to 2.2-log increase in the number of bone marrow-derived antibody-secreting cells compared to the RBD formulated with Alum without an additional agonist. In contrast, the RBD formulated with SE in combination with 3M-052 or CpG did not elicit an IgG response greater than the unadjuvanted control. Additionally, RBD formulated with 3M-052 or CpG on Alum generated a 0.8- or 1.6-log lower splenocyte IL-5 response (a pro-Th2 marker), respectively, than Alum without an additional agonist. When formulated with 3M-052-Alum, a bivalent vaccine containing the original lineage (Wuhan-Hu-1) and the Delta variant (B.1.617.2) RBD antigens led to a more than 2-log increase in neutralizing antibodies against an Omicron variant (B.1.1.529) pseudovirus in vaccinated animals compared to animals that received the monovalent RBD antigen.

Discussion: Our results suggest that optimal immune responses to subunit antigens may be achieved through an orthogonal approach that applies adjuvant formulation, antigen combination, and advances in rational vaccine development techniques.

Keywords

receptor binding domain, adjuvant formulation, SARS-CoV-2, vaccine development, toll-like receptor, bivalent vaccine

Published Open-Access

yes

Recommended Citation

Lykins, William R; Pollet, Jeroen; White, Jessica A; et al., "Choice of Adjuvant and Antigen Composition Alters the Immunogenic Profile of a SARS-CoV-2 Subunit Vaccine" (2024). Faculty and Staff Publications. 5867.
https://digitalcommons.library.tmc.edu/baylor_docs/5867