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Application of Phosphorylcholine Derivative As Mucosal Adjuvant Enhancing Mucosal Immune Responses in the Upper Respiratory Tract

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Date 2023 Aug 2
PMID 37532644
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Abstract

Objective: A phosphorylcholine (PC)-derivative with high binding ability (PCDB) was intranasally administered to mice with ovalbumin (OVA), and immune responses were investigated to determine whether PCDB has antigenicity and adjuvanticity.

Methods: BALB/c mice were intranasally immunized with PCDB coupled with OVA, unbound PCDB plus OVA, cholera toxin (CT) plus OVA, OVA alone, and PCDB alone. Then, the production of OVA- and PC-specific antibodies in external secretions and serum, and the secretion of cytokines such as IL-4 and IFN-γ from splenic mononuclear cells by stimulation with PCDB and OVA were examined. Furthermore, the secretion of IL-12p40 from CD11c cells following stimulation with PCDB was observed to clarify the adjuvant effect of PCDB through TLR4.

Results: Intranasal immunization with PCDB plus OVA increased OVA- and PC-specific IgA in external secretions and OVA- and PC-specific antibodies in the serum. The analysis of IgG subclasses specific to OVA and PC showed a higher production of IgG1 than IgG2, and the secretion of both IL-4 and IFN-γ was enhanced. However, IL-12p40 secretion from CD11c cells was increased and OVA-specific IgE production was not promoted by PCDB stimulation.

Conclusion: Intranasal administration of the protein antigen with PCDB enhanced immune responses specific to the mixed antigen and PC. Although PCDB acted to bias the immune response toward the Th2-type, antigen-specific IgE production did not increase. These findings suggest that PCDB has the potential to be a mucosal vaccine with both adjuvanticity and antigenicity without causing side effects due to type I allergy.

Citing Articles

Broad specificity of monoclonal IgA (TEPC15-IgA) for enteric bacteria via phosphorylcholine-mediated interaction.

Koyama S, Ito K, Usami K, Wada S, Yamashita T, Ikeda-Ohtsubo W J Vet Med Sci. 2024; 86(7):801-808.

PMID: 38839348 PMC: 11251817. DOI: 10.1292/jvms.23-0441.