A chimeric thermostable M2e and H3 stalk-based universal influenza A virus vaccine

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Jeeva Subbiah
Judy Oh
Ki-Hye Kim
Chong-Hyun Shin
Bo Ryoung Park
Noopur Bhatnagar
Baik-Lin Seong
Bao-Zhong Wang
Sang-Moo Kang
机构
[1] Georgia State University,Center for Inflammation, Immunity & Infection, Institute for Biomedical Sciences
[2] Yonsei University,Department of Microbiology, College of Medicine
[3] Vaccine Innovative Technology ALliance (VITAL)-Korea,undefined
[4] Yonsei University,undefined
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We developed a new chimeric M2e and H3 hemagglutinin (HA) stalk protein vaccine (M2e-H3 stalk) by genetic engineering of modified H3 stalk domain conjugated with conserved M2e epitopes to overcome the drawbacks of low efficacy by monomeric domain-based universal vaccines. M2e-H3 stalk protein expressed and purified from Escherichia coli was thermostable, displaying native-like antigenic epitopes recognized by antisera of different HA subtype proteins and influenza A virus infections. Adjuvanted M2e-H3 stalk vaccination induced M2e and stalk-specific IgG antibodies recognizing viral antigens on virus particles and on the infected cell surface, CD4+ and CD8+ T-cell responses, and antibody-dependent cytotoxic cell surrogate activity in mice. M2e-H3 stalk was found to confer protection against heterologous and heterosubtypic cross-group subtype viruses (H1N1, H5N1, H9N2, H3N2, H7N9) at similar levels in adult and aged mice. These results provide evidence that M2e-H3 stalk chimeric proteins can be developed as a universal influenza A virus vaccine candidate for young and aged populations.
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