AI Article Synopsis

  • Intramuscular inactivated influenza vaccines are the standard for preventing seasonal flu, but H5N1 vaccines have lower effectiveness despite being safe.
  • Needle-free and mucosal vaccination methods could improve efficiency in pandemics, and PIKA, a chemical adjuvant, has shown promise in enhancing the immune response in mouse models.
  • PIKA works by increasing the number of mature immune cells and cytokine production, and its effectiveness relies on TLR3, making it a potential game-changer for future vaccine strategies against H5N1.

Article Abstract

Intramuscular administration of inactivated influenza virus vaccine is the main vaccine platform used for the prevention of seasonal influenza virus infection. In clinical trials, inactivated H5N1 vaccines have been shown to be safe and capable of eliciting immune correlates of protection. However, the H5N1 vaccines are poorly immunogenic compared to seasonal influenza virus vaccines. Needle-free vaccination would be more efficient and economical in a pandemic, and the development of an effective and safe mucosal adjuvant will be an important milestone. A stabilized chemical analog of double-stranded RNA, PIKA, was previously reported to be a potent mucosal adjuvant in a murine model. While PIKA stimulates dendritic cells in vitro, little was known about its receptor and adjuvanting mechanism in vivo. In this study, we demonstrated that the immunostimulatory effect of PIKA resulted in an increased number of mature antigen-presenting cells, with the induction of proinflammatory cytokines at the inoculation site. In addition, coadministration of PIKA with a poorly immunogenic H5N1 subunit vaccine led to antigen sparing and quantitative and qualitative improvements of the immune responses over those achieved with an unadjuvanted vaccine in mice. The adjuvanted vaccine provided protection against lethal challenge with homologous and heterologous H5N1 wild-type viruses. Mice lacking functional TLR3 showed diminished cytokine production with PIKA stimulation, diminished antibody responses, and reduced protective efficacy against wild-type virus challenge following vaccination. These data suggest that TLR3 is important for the optimal performance of PIKA as an adjuvant. With its good safety profile and antigen-sparing effect, PIKA could be an attractive adjuvant for use in future pandemics.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC2919013PMC
http://dx.doi.org/10.1128/JVI.00596-10DOI Listing

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