Intranasal immunization using biphasic lipid vesicles as delivery systems for OmlA bacterial protein antigen and CpG oligonucleotides adjuvant in a mouse model

Author:

Alcón V L12,Baca-Estrada M1,Vega-López M A1,Willson P1,Babiuk L A1,Kumar P3,Foldvari M2

Affiliation:

1. Vaccine and Infectious Disease Organization, University of Saskatchewan, Saskatoon, Canada S7N 5E3

2. College of Pharmacy and Nutrition, University of Saskatchewan, Saskatoon, Canada S7N 5E3

3. PharmaDerm Laboratories Ltd, Innovation Place Research Park, Saskatoon, Canada

Abstract

Abstract The nasal mucosa is an important arm of the mucosal system since it is often the first point of contact for inhaled antigens. The ineffectiveness of the simple delivery of soluble antigens to mucosal membranes for immunization has stimulated extensive studies in appropriate delivery systems and adjuvants. We have evaluated biphasic lipid vesicles as a novel intranasal (i.n.) delivery system (designated as vaccine targeting adjuvant, VTA) containing bacterial antigens and CpG oligode-oxynucleotides (ODNs). Results show that administration of antigen and CpG ODNs in biphasic lipid vesicles resulted in greater induction of IgA levels in serum (P<0.05) and mucosal antibody responses such as IgA in nasal secretions and lung (P<0.01) after immunization with a combined subcutaneous (s.c.)/i.n. as compared to s.c./s.c. approach. Based on antibody responses, VTA formulations were found to be suitable as delivery systems for antigens and CpG ODNs by the intranasal route, resulting in a Th2-type of immune response, characterized by IgG1 and IL-4 production at the systemic level.

Publisher

Oxford University Press (OUP)

Subject

Pharmaceutical Science,Pharmacology

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