Evaluation of Efficacy of Surface Coated versus Encapsulated Influenza Antigens in Mannose–Chitosan Nanoparticle-Based Intranasal Vaccine in Swine
Author | Bugybayeva, Dina |
Author | Dumkliang, Ekachai |
Author | Patil, Veerupaxagouda |
Author | Yadagiri, Ganesh |
Author | Suresh, Raksha |
Author | Singh, Mithilesh |
Author | Schrock, Jennifer |
Author | Dolatyabi, Sara |
Author | Shekoni, Olaitan C. |
Author | Yassine, Hadi M. |
Author | Opanasopit, Praneet |
Author | HogenEsch, Harm |
Author | Renukaradhya, Gourapura J. |
Available date | 2024-11-03T07:51:38Z |
Publication Date | 2024-06-11 |
Publication Name | Vaccines |
Identifier | http://dx.doi.org/10.3390/vaccines12060647 |
Citation | Bugybayeva, D., Dumkliang, E., Patil, V., Yadagiri, G., Suresh, R., Singh, M., ... & Renukaradhya, G. J. (2024). Evaluation of Efficacy of Surface Coated versus Encapsulated Influenza Antigens in Mannose–Chitosan Nanoparticle-Based Intranasal Vaccine in Swine. Vaccines, 12(6), 647. |
Abstract | This study focuses on the development and characterization of an intranasal vaccine platform using adjuvanted nanoparticulate delivery of swine influenza A virus (SwIAV). The vaccine employed whole inactivated H1N2 SwIAV as an antigen and STING-agonist ADU-S100 as an adjuvant, with both surface adsorbed or encapsulated in mannose–chitosan nanoparticles (mChit-NPs). Optimization of mChit-NPs included evaluating size, zeta potential, and cytotoxicity, with a 1:9 mass ratio of antigen to NP demonstrating high loading efficacy and non-cytotoxic properties suitable for intranasal vaccination. In a heterologous H1N1 pig challenge trial, the mChit-NP intranasal vaccine induced cross-reactive sIgA antibodies in the respiratory tract, surpassing those of a commercial SwIAV vaccine. The encapsulated mChit-NP vaccine induced high virus-specific neutralizing antibody and robust cellular immune responses, while the adsorbed vaccine elicited specific high IgG and hemagglutinin inhibition antibodies. Importantly, both the mChit-NP vaccines reduced challenge heterologous viral replication in the nasal cavity higher than commercial swine influenza vaccine. In summary, a novel intranasal mChit-NP vaccine platform activated both the arms of the immune system and is a significant advancement in swine influenza vaccine design, demonstrating its potential effectiveness for pig immunization. |
Sponsor | This work was supported by United States Department of Agriculture, National Institute of Food and Agriculture (USDA-NIFA), Agriculture and Food Research Initiative (AFRI) grant #2019-67015-29814 and #2019-67015-29815. Some part of this research collaboration between the USA and Thailand was financed by the National Research Council of Thailand (NRCT) through the Golden Jubilee Ph.D. Program (Contact No. PHD/0194/2561) and the National Vaccine Institute of Thailand (Contact No. 2563.1/5). |
Language | en |
Publisher | Multidisciplinary Digital Publishing Institute (MDPI) |
Subject | adjuvanted vaccine cellular immunity H1N2 swine influenza virus intranasal vaccination mannose–chitosan nanoparticles |
Type | Article |
Issue Number | 6 |
Volume Number | 12 |
ESSN | 2076-393X |
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