Literature DB >> 33746943

Immunity and Protective Efficacy of Mannose Conjugated Chitosan-Based Influenza Nanovaccine in Maternal Antibody Positive Pigs.

Sankar Renu1,2, Ninoshkaly Feliciano-Ruiz1,2, Veerupaxagouda Patil1,2, Jennifer Schrock1,2, Yi Han1,2, Anikethana Ramesh1,2, Santosh Dhakal1,2, Juliette Hanson1,2, Steven Krakowka3, Gourapura J Renukaradhya1,2.   

Abstract

Parenteral administration of killed/inactivated swine influenza A virus (SwIAV) vaccine in weaned piglets provides variable levels of immunity due to the presence of preexisting virus specific maternal derived antibodies (MDA). To overcome the effect of MDA on SwIAV vaccine in piglets, we developed an intranasal deliverable killed SwIAV antigen (KAg) encapsulated chitosan nanoparticles called chitosan-based NPs encapsulating KAg (CS NPs-KAg) vaccine. Further, to target the candidate vaccine to dendritic cells and macrophages which express mannose receptor, we conjugated mannose to chitosan (mCS) and formulated KAg encapsulated mCS nanoparticles called mannosylated chitosan-based NPs encapsulating KAg (mCS NPs-KAg) vaccine. In MDA-positive piglets, prime-boost intranasal inoculation of mCS NPs-KAg vaccine elicited enhanced homologous (H1N2-OH10), heterologous (H1N1-OH7), and heterosubtypic (H3N2-OH4) influenza virus-specific secretory IgA (sIgA) antibody response in nasal passage compared to CS NPs-KAg vaccinates. In vaccinated upon challenged with a heterologous SwIAV H1N1, both mCS NPs-KAg and CS NPs-KAg vaccinates augmented H1N2-OH10, H1N1-OH7, and H3N2-OH4 virus-specific sIgA antibody responses in nasal swab, lung lysate, and bronchoalveolar lavage (BAL) fluid; and IgG antibody levels in lung lysate and BAL fluid samples. Whereas, the multivalent commercial inactivated SwIAV vaccine delivered intramuscularly increased serum IgG antibody response. In mCS NPs-KAg and CS NPs-KAg vaccinates increased H1N2-OH10 but not H1N1-OH7 and H3N2-OH4-specific serum hemagglutination inhibition titers were observed. Additionally, mCS NPs-KAg vaccine increased specific recall lymphocyte proliferation and cytokines IL-4, IL-10, and IFNγ gene expression compared to CS NPs-KAg and commercial SwIAV vaccinates in tracheobronchial lymph nodes. Consistent with the immune response both mCS NPs-KAg and CS NPs-KAg vaccinates cleared the challenge H1N1-OH7 virus load in upper and lower respiratory tract more efficiently when compared to commercial vaccine. The virus clearance was associated with reduced gross lung lesions. Overall, mCS NP-KAg vaccine intranasal immunization in MDA-positive pigs induced a robust cross-reactive immunity and offered protection against influenza virus.
Copyright © 2021 Renu, Feliciano-Ruiz, Patil, Schrock, Han, Ramesh, Dhakal, Hanson, Krakowka and Renukaradhya.

Entities:  

Keywords:  chitosan nanoparticle; immune response; intranasal vaccination; mannose; maternally derived antibodies; pigs; swine influenza virus

Mesh:

Substances:

Year:  2021        PMID: 33746943      PMCID: PMC7969509          DOI: 10.3389/fimmu.2021.584299

Source DB:  PubMed          Journal:  Front Immunol        ISSN: 1664-3224            Impact factor:   7.561


  58 in total

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Authors:  Santosh Dhakal; Sankar Renu; Shristi Ghimire; Yashavanth Shaan Lakshmanappa; Bradley T Hogshead; Ninoshkaly Feliciano-Ruiz; Fangjia Lu; Harm HogenEsch; Steven Krakowka; Chang Won Lee; Gourapura J Renukaradhya
Journal:  Front Immunol       Date:  2018-05-02       Impact factor: 7.561

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Journal:  Int J Nanomedicine       Date:  2020-02-03
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