Background: Invasive meningococcal disease (IMD), caused by Neisseria meningitidis, is a public health problem, associated with high levels of morbidity and mortality, capable of causing outbreaks or epidemics, but preventable through vaccination. In Brazil, the main serogroups isolated are C and B. The last epidemic occurred in the 80s, in Sao Paulo, because of a B:4:P1.15 strain. Methods: Adult Swiss mice were immunized with outer membrane vesicles (OMV) of N. meningitidis strain C:4:P1.15, adjuvanted by the cationic lipid dioctadecyldimethylammonium bromide in bilayer fragments (DDA-BF), administered via prime-booster (intranasal/subcutaneous) scheme. The humoral response was accessed by Immunoblotting and ELISA, using homologous immunization strain and a different serogroup but equal serosubtype strain, N. meningitidis B:4:P1.15. Results: Immunoblotting revealed the recognition of antigens associated with the molecular weight of Porin A and Opacity proteins, which are immunogenic but highly heterogeneous, and Tbp and NspA, which are more homogeneous between meningococci strains. ELISA results showed antibody production that persisted after 190 days and recognized the C:4:P1.15 and the B:4:P1.15 strains, with high avidity index. The adjuvanted group recognized antigens following the IN prime and had a higher avidity index against the heterologous strain. Conclusions: DDA-BF improved the humoral response, but the OMV alone induced high avidity index antibodies as well. Even though these are preliminary results, we see it as a promising approach for affordable meningococcal immunization in developing countries, at outbreak or epidemic situations.
Introduction: Neisseria meningitidis causes Invasive Meningococcal Disease (IMD). Immunization should achieve a persistent immune response against pathogens, at local and systemic levels, which can be modulated by administration site and appropriate adjuvants. Dimethyldioctadecylammonium bromide is a cationic lipid with adjuvant properties that can be used in as vesicles (DDA) or bilayer fragments (DDA-BF). Prime-booster scheme induces local and systemic antibodies.Objective: Testing the persistence of antibodies triggered by immunization with outer membrane vesicles (OMV) of N. meningitidis C:4:P1.15, complexed with DDA or DDA-BF, against homologous and B:4:P1.15 strain, representative of the last epidemic period of IMD in Brazil.Methodology: Antigenic preparations containing 0.25µg OMV+0.1mM DDA; 0.25µg OMV+0.01mM DDA-BF; 0.25µg OMV; 0.1mM DDA or 0.1mM DDA-BF were intranasally administered in adult Swiss mice on days 1, 2, 22 and 23. A subcutaneous booster containing 5µg OMV+0,1mM DDA; 5µg OMV+0.01mM DDA-BF, 5µg OMV; 0.1mM DDA or 0.1mM DDA-BF was administered on day 41. Blood was taken before immunization (pre-immune) and 180 days after the booster dose. ELISA plates (MaxSorp, Nunc) were coated with whole cells suspensions of strains C:4:P1.15 or B:4:P1.15 at an optical density (OD) 0.1 at 620nm. Serum samples at 1:50 were incubated for 2 hours at 37°C. Anti-IgG γ chain (Kirkegaard & Perry Laboratories) at 1:20,000 was incubated for 2 hours at 37°C. The reaction was revealed with the addition of tetramethylbenzidine for 20 minutes at 37°C, stopped with 1N sulfuric acid and read at 450nm (Molecular Devices). Results were analyzed using One-Way ANOVA method followed by Tukey's post-test (GraphPad Prism 8). The Avidity Index (AI) was performed by a modified ELISA using 1.5M potassium thiocyanate (KSCN) as a chaotropic agent and expressed as the ratio between OD with KSCN/without KSCN and considered high if AI>0.5, intermediate if . 0.5>AI>0.3 or low if AI<0.3.Results: Against C:4:P1.15 strain, higher ODs were observed in immune samples when compared to the pre-immune and adjuvant controls, but there was no statistical difference between the groups. For B:4:P1.15 strain, when compared to the pre-immune control, the groups OMV (p=0.0342) and OMV+DDA-BF (p=0.0219) showed a statistical difference. However, all the individuals of OMV+DDA; OMV+DDA-BF and OMV groups showed high AI against C:4:P1.15, as well against B:4:P1.15, except for one individual from the OMV+DDA group who had intermediate avidity. Conclusion:The immunization scheme was able to induce a persistent humoral response, with antibodies capable of binding to strains C:4:P1.15 and B:4:P1.15 with high AI. DDA-BF seems better than DDA as adjuvant. The group immunized with OMV showed a similar response to the groups with adjuvants in the preparation, suggesting that the strain itself is immunogenic. Functionality assays, as serum bactericidal activity should be enrolled to verify the protective potential.
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