Retinoic acid-adjuvanted vaccine induces antigen-specific secretory IgA in the gut of newborn piglets

Gitte Erbs; Jeanne Toft Jakobsen; Signe Tandrup Schmidt; Dennis Christensen; Mick Bailey; Gregers Jungersen

doi:10.1016/j.vaccine.2024.126672

Retinoic acid-adjuvanted vaccine induces antigen-specific secretory IgA in the gut of newborn piglets

Vaccine. 2024 Dec 28:46:126672. doi: 10.1016/j.vaccine.2024.126672. Online ahead of print.

Authors

Gitte Erbs¹, Jeanne Toft Jakobsen¹, Signe Tandrup Schmidt¹, Dennis Christensen¹, Mick Bailey², Gregers Jungersen³

Affiliations

¹ Infectious Disease Immunology, Center for Vaccine Research, SSI, Copenhagen, Denmark.
² Bristol Veterinary School, Langford House, University of Bristol, UK.
³ Infectious Disease Immunology, Center for Vaccine Research, SSI, Copenhagen, Denmark. Electronic address: [email protected].

PMID: 39733479
DOI: 10.1016/j.vaccine.2024.126672

Abstract

Mucosal secretory IgA (SIgA) produced by subepithelial plasma cells in the lamina propria is the major antigen-specific defense mechanism against mucosal infections. We investigated if a retinoic acid (RA)-containing adjuvant in parenteral immunization, can induce vaccine-specific SIgA in the jejunal lumen in a dose-dependent manner in neonatal pigs immunized with a Chlamydia hybrid antigen. To accurately quantify SIgA responses in mucosal secretions, an antigen-specific ELISA method with secondary detection of porcine secretory component rather than IgA was developed. RA facilitated a stronger (or faster) IgG, IgA, IgM and SIgA response in serum after primary immunization, and a more than 10-fold significantly increased level of vaccine-specific SIgA in jejunum at termination 2 weeks after the secondary boost, whereas IgA or SIgA responses in bronchoalveolar lavage (BAL) were not significantly increased after immunization with RA. Analyses of different isotype responses to vaccination and different sampling sites, revealed significant correlations between IgG and IgA responses in serum, and between IgG in serum and jejunum, while IgA in jejunum was neither correlated with IgA in serum nor with IgG in jejunum. This is indicative of IgG in jejunum being primarily a transudate from serum, while IgA is not. Jejunum SIgA correlated significantly with jejunum IgA and with both serum SIgA and IgA. Our results thus support the use of SC-specific reagents for mucosal SIgA responses, although IgA reagents to a lesser extent also reflects local antibodies. Although the IgA and SIgA levels in BAL were not significantly different with or without RA, we observed a significant correlation of vaccine-specific SIgA in jejunum and BAL, indicating a level of commonality in the regulation of mucosal antibodies in gut and respiratory system. In conclusion, an adjuvant with high concentration of RA was shown to increase the local intestinal mucosal antibody response after parenteral immunization in pigs.

Keywords: ELISA; Mucosal immunity; Neonatal; Pig; Retinoic acid; Secretory IgA; Vaccine.