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A bivalent Mpox nanoparticle vaccine induces robust immune response and provides long-lasting protection against vaccinia virus challenge

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NIAID Data Ecosystem2026-05-02 收录
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https://figshare.com/articles/dataset/A_bivalent_Mpox_nanoparticle_vaccine_induces_robust_immune_response_and_provides_long-lasting_protection_against_vaccinia_virus_challenge/29657267
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The 2022 and 2024 monkeypox (mpox) outbreak highlighted the urgent need for effective, durable, and safe vaccines. In addition to the traditional smallpox vaccines that could bring cross-protection against mpox, mRNA and protein-subunit mpox vaccines were extensively studied after the outbreak of mpox. In this study, we engineered monkeypox virus (MPXV) nanoparticle vaccines by conjugating the M1R and A35R, two well-characterized protective antigens to the mi3 nanoparticle using the SpyTag-SpyCatcher system, generating mi3-M1R and mi3-A35R constructs. An equimolar mixture of mi3-M1R and mi3-A35R formed a bivalent MPXV vaccine candidate, termed mi3-AM. When administered intraperitoneally with the Mn adjuvant, the mi3-AM vaccine induced robust humoral and antigen-specific cellular immune responses. Notably, the mi3-AM vaccine provided long-lasting protection against a lethal challenge with vaccinia virus Western Reserve strain (VACV-WR) in mice. With ongoing mpox outbreaks and the limitations of current vaccines, our candidate represents a promising, deployable solution with potential to bridge existing gaps in global orthopoxvirus prevention.
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2025-07-28
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