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Polycationic HA/CpG Nanoparticles Induce Cross-Protective Influenza Immunity in Mice

Chunhong Dong, Ye Wang, Wandi Zhu, Yao Ma, Joo Hee Kim, Lai Wei, Gilbert X. Gonzalez, Bao‐Zhong Wang

2022ACS Applied Materials & Interfaces39 citationsDOIOpen Access PDF

Abstract

The intranasal (i.n.) route is an ideal vaccination approach for infectious respiratory diseases like influenza. Polycationic polyethylenimine (PEI) could form nanoscale complexes with negatively charged viral glycoproteins. Here we fabricated PEI-hemagglutinin (HA) and PEI-HA/CpG nanoparticles and investigated their immune responses and protective efficacies with an i.n. vaccination regimen in mice. Our results revealed that the nanoparticles significantly enhanced HA immunogenicity, providing heterologous cross-protection. The conserved HA stalk region induced substantial antibodies in the nanoparticle immunization groups. In contrast to the Th2-biased, IgG1-dominant antibody response generated by PEI-HA nanoparticles, PEI-HA/CpG nanoparticles generated more robust and balanced IgG1/IgG2a antibody responses with augmented neutralization activity and Fc-mediated antibody-dependent cellular cytotoxicity (ADCC). PEI-HA/CpG nanoparticles also induced enhanced local and systemic cellular immune responses. These immune responses did not decay over six months of observation postimmunization. PEI and CpG synergized these comprehensive immune responses. Thus, the PEI-HA/CpG nanoparticle is a potential cross-protective influenza vaccine candidate. Polycationic PEI nanoplatforms merit future development into mucosal vaccine systems.

Topics & Concepts

ImmunogenicityImmune systemCpG OligodeoxynucleotidePolyethylenimineAntibodyAntibody-dependent cell-mediated cytotoxicityHemagglutinin (influenza)ImmunopotentiatorVaccinationImmunizationCytotoxicityAdjuvantVirologyBiologyMaterials scienceImmunologyCell cultureBiochemistryIn vitroGene expressionTransfectionMonoclonal antibodyGeneticsDNA methylationGeneInfluenza Virus Research StudiesImmunotherapy and Immune ResponsesImmune Response and Inflammation
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