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Improved adjuvanting of seasonal influenza vaccines: Preclinical studies of MVA‐NP+M1 coadministration with inactivated influenza vaccine
Authors:Caitlin E. Mullarkey  Amy Boyd  Arjan van Laarhoven  Eric A. Lefevre  B. Veronica Carr  Massimiliano Baratelli  Eleonora Molesti  Nigel J. Temperton  Colin Butter  Bryan Charleston  Teresa Lambe  Sarah C. Gilbert
Affiliation:1. Jenner Institute, Old Road Campus Research Building, , Oxford, UK;2. Pirbright Institute, Compton laboratory, , Compton, UK;3. Centre de Recerca en Sanitat Animal (CReSA), , Barcelona, Spain;4. Viral Pseudotype Unit, Medway School of Pharmacy, University of Kent, Chatham Maritime, , Kent, UK
Abstract:Licensed seasonal influenza vaccines induce antibody (Ab) responses against influenza hemagglutinin (HA) that are limited in their ability to protect against different strains of influenza. Cytotoxic T lymphocytes recognizing the conserved internal nucleoprotein (NP) and matrix protein (M1) are capable of mediating a cross‐subtype immune response against influenza. Modified vaccinia Ankara (MVA) virus encoding NP and M1 (MVA‐NP+M1) is designed to boost preexisting T‐cell responses in adults in order to elicit a cross‐protective immune response. We examined the coadministration of HA protein formulations and candidate MVA‐NP+M1 influenza vaccines in murine, avian, and swine models. Ab responses postimmunization were measured by ELISA and pseudotype neutralization assays. Here, we demonstrate that MVA‐NP+M1 can act as an adjuvant enhancing Ab responses to HA while simultaneously inducing potent T‐cell responses to conserved internal Ags. We show that this regimen leads to the induction of cytophilic Ab isotypes that are capable of inhibiting hemagglutination and in the context of H5 exhibit cross‐clade neutralization. The simultaneous induction of T cells and Ab responses has the potential to improve seasonal vaccine performance and could be employed in pandemic situations.
Keywords:Adjuvants  Influenza vaccines  T cells  Vaccination
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