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Impact of hemagglutination activity and M2e immunity on conferring protection against influenza viruses.


ABSTRACT: To improve cross-protection of influenza vaccination, we tested conjugation of conserved M2e epitopes to the surface of inactivated influenza virus (iPR8-M2e*). Treatment of virus with chemical cross-linker led to diminished hemagglutination activity and failure to induce hemagglutination inhibiting antibodies. Conjugated iPR8-M2e* vaccine was less protective against homologous and heterosubtypic viruses, despite the induction of virus-specific binding IgG antibodies. In alternative approaches to enhance cross-protection, we developed a genetically linked chimeric protein (M2e-B stalk) vaccine with M2e of influenza A and hemagglutinin (HA) stalk of influenza B virus. Vaccination of mice with inactivated influenza A virus supplemented with M2e-B stalk effectively induced hemagglutination inhibiting antibodies, humoral and cellular M2e immune responses, and enhanced heterosubtypic protection. This study demonstrates the importance of HA functional integrity in influenza vaccine efficacy and that supplementation of influenza vaccines with M2e-B stalk protein could be a feasible strategy of improving cross-protection against influenza viruses.

SUBMITTER: Oh J 

PROVIDER: S-EPMC9978532 | biostudies-literature | 2022 Sep

REPOSITORIES: biostudies-literature

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Impact of hemagglutination activity and M2e immunity on conferring protection against influenza viruses.

Oh Judy J   Subbiah Jeeva J   Kim Ki-Hye KH   Park Bo Ryoung BR   Bhatnagar Noopur N   Garcia Karla Ruiz KR   Liu Rong R   Jung Yu-Jin YJ   Shin Chong-Hyun CH   Seong Baik-Lin BL   Kang Sang-Moo SM  

Virology 20220716


To improve cross-protection of influenza vaccination, we tested conjugation of conserved M2e epitopes to the surface of inactivated influenza virus (iPR8-M2e*). Treatment of virus with chemical cross-linker led to diminished hemagglutination activity and failure to induce hemagglutination inhibiting antibodies. Conjugated iPR8-M2e* vaccine was less protective against homologous and heterosubtypic viruses, despite the induction of virus-specific binding IgG antibodies. In alternative approaches t  ...[more]

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