Intranasal G5‐BGG/pDNA Vaccine Elicits Protective Systemic and Mucosal Immunity against SARS‐CoV‐2 by Transfecting Mucosal Dendritic Cells

Author:

Zhang Han1,Liu Zezhong2,Lihe Hongye1,Lu Linwei34,Zhang Zongxu1,Yang Shengmin1,Meng Nana1,Xiong Yin1,Fan Xingyan1,Chen Zhikai2,Lu Weiyue156,Xie Cao6,Liu Min1ORCID

Affiliation:

1. Department of Pharmaceutics and the Key Laboratory of Smart Drug Delivery Ministry of Education School of Pharmacy Fudan University Shanghai 201203 China

2. Department of Pharmacology and the Key Laboratory of Smart Drug Delivery Ministry of Education School of Pharmacy Fudan University Shanghai 201203 China

3. Department of Integrative Medicine Huashan Hospital Fudan University Shanghai 201203 China

4. Institutes of Integrative Medicine Fudan University Shanghai 201203 China

5. Shanghai Engineering Technology Research Center for Pharmaceutica Intelligent Equipment Shanghai Frontiers Science Center for Druggability of Cardiovascular non‐coding RNA Institute for Frontier Medical Technology Shanghai University of Engineering Science Shanghai 201203 China

6. Shanghai Tayzen Pharmlab Co., Ltd. Shanghai 201203 China

Abstract

AbstractInfectious disease pandemics, including the coronavirus disease 2019 pandemic, have heightened the demand for vaccines. Although parenteral vaccines induce robust systemic immunity, their effectiveness in respiratory mucosae is limited. Considering the crucial role of nasal‐associated lymphoid tissue (NALT) in mucosal immune responses, in this study, the intranasal complex composed of G5‐BGG and antigen‐expressing plasmid DNA (pSP), named G5‐BGG/pSP complex, is developed to activate NALT and to promote both systemic and mucosal immune defense. G5‐BGG/pSP could traverse mucosal barriers and deliver DNA to the target cells because of its superior nasal retention and permeability characteristics. The intranasal G5‐BGG/pSP complex elicits robust antigen‐specific immune responses, such as the notable production of IgG antibody against several virus variants. More importantly, it induces elevated levels of antigen‐specific IgA antibody and a significant expansion of the lung‐resident T lymphocyte population. Notably, the intranasal G5‐BGG/pSP complex results in antigen expression and maturation of dendritic cells in nasal mucosae. These findings exhibit the potential of G5‐BGG, a novel cationic material, as an effective gene carrier for intranasal vaccines to obtain robust systemic and mucosal immunity.

Funder

National Natural Science Foundation of China

Publisher

Wiley

Subject

Pharmaceutical Science,Biomedical Engineering,Biomaterials

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