AI Article Synopsis

  • Next generation influenza vaccines targeting conserved epitopes have the potential to improve pandemic readiness and long-term protection but face challenges related to virus adaptation and immune escape.
  • Key strategies include HA-stem and T cell activating vaccines, which may unintentionally promote residual virus survival by recognizing the virus after it enters cells, necessitating pre-emptive immune priming.
  • To effectively enhance T cell responses, innovative methods like viral vectors and peptide approaches are essential, particularly since current live attenuated vaccines lack sufficient immunogenicity in adults with prior immunity.

Article Abstract

Next generation influenza vaccines that target conserved epitopes are becoming a clinical reality but still have challenges to overcome. Universal next generation vaccines are considered a vital tool to combat future pandemic viruses and have the potential to vastly improve long-term protection against seasonal influenza viruses. Key vaccine strategies include HA-stem and T cell activating vaccines; however, they could have unintended effects for virus adaptation as they recognise the virus after cell entry and do not directly block infection. This may lead to immune pressure on residual viruses. The potential for immune escape is already evident, for both the HA stem and T cell epitopes, and mosaic approaches for pre-emptive immune priming may be needed to circumvent key variants. Live attenuated influenza vaccines have not been immunogenic enough to boost T cells in adults with established prior immunity. Therefore, viral vectors or peptide approaches are key to harnessing T cell responses. A plethora of viral vector vaccines and routes of administration may be needed for next generation vaccine strategies that require repeated long-term administration to overcome vector immunity and increase our arsenal against diverse influenza viruses.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC8472936PMC
http://dx.doi.org/10.3390/v13091779DOI Listing

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