Protective efficacy of a universal influenza mRNA vaccine against the challenge of H1 and H5 influenza A viruses in mice

Author:

Li Yulei12ORCID,Wang Xi3,Zeng Xi4,Ren Wenbo5,Liao Pu6,Zhu Baoli378ORCID

Affiliation:

1. Savaid Medical School University of Chinese Academy of Sciences Beijing China

2. The Key Laboratory of Molecular Pathology (Hepatobiliary Diseases) of Guangxi, Department of Pathology The Affiliated Hospital of Youjiang Medical University for Nationalities Baise China

3. CAS Key Laboratory of Pathogenic Microbiology and Immunology Chinese Academy of Sciences Beijing China

4. Beijing Children's Hospital Capital Medical University Beijing China

5. College of Life Sciences Jiangxi Science and Technology Normal University Nanchang China

6. Department of Clinical Laboratory Chongqing General Hospital Chongqing China

7. University of Chinese Academy of Sciences Beijing China

8. Department of Pathogenic Biology, School of Basic Medical Sciences Southwest Medical University Luzhou China

Abstract

AbstractCurrent influenza vaccines need to be updated annually owing to constant antigenic drift in the globular head of the viral surface hemagglutinin (HA) glycoprotein. The immunogenic subdominant stem domain of HA is highly conserved and can be recognized by antibodies capable of binding multiple HA subtypes. Therefore, the HA stem antigen is a promising target for the design of universal influenza vaccines. On the basis of an established lipid nanoparticle‐encapsulated mRNA vaccine platform, we designed and developed a novel universal influenza mRNA vaccine (mHAs) encoding the HA stem antigen of the influenza A (H1N1) virus. We tested the efficacy of the mHAs vaccine using a mouse model. The vaccine induced robust humoral and specific cellular immune responses against the stem region of HA. Importantly, two doses of the mHAs vaccine fully protected mice from lethal challenges of the heterologous H1N1 and heterosubtypic H5N8 influenza viruses. Vaccinated mice had less pathological lung damage and lower viral titers than control mice. These results suggest that an mRNA vaccine using the conserved stem region of HA may provide effective protection against seasonal and other possible influenza variants.

Publisher

Wiley

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