Furthermore, more pathogenic viruses such as the newly emerged pandemic H1N1 virus of 2009 (pH1N1/09)
for which among others, relatively young people were at an increased risk, highlight the need for improved influenza vaccines that induce better, more cross-protective, and longer lasting immunity than the current seasonal vaccines do. Vaccines administered parenterally induce effective systemic immune responses, but only limited local immunity in the respiratory tract. Locally produced High Content Screening specific antibodies, in particular secretory IgA (S-IgA) can provide immunity via their unique capability to neutralize a pathogen before it even passes the mucosal barrier [4] and [5]. Moreover S-IgA antibodies have been demonstrated to contribute to the establishment of increased cross-protection from influenza [6]. Nasal administration of vaccine has the potential of establishing mucosal immune responses at the first site of natural infection [7]. In addition, nasal administration using a needle free delivery system is non-invasive, simply
accessible and painless. The currently licensed nasally administered influenza vaccines are live attenuated influenza vaccines KU57788 (LAIV). The LAIV vaccine manufactured by Medimmune, sold under the trade name FluMist in the US and Fluenz in Europe, has proven to be effective against seasonal infection and to provide better cross-protection against drifted influenza virus strains than the non-live seasonal vaccines [8], [9] and [10]. However, the use of LAIV is currently restricted to the age group of 2 to 59 years, thus excluding
children below age 2 as well as the elderly, both populations classified as major high risk groups by the WHO [2]. Therefore, nasal administration of an inactivated influenza vaccine that would be safe and protective through systemic and mucosal immunity, would be an attractive alternative to currently used influenza vaccines. Appropriate Dipeptidyl peptidase adjuvants or carrier systems have shown to be indispensable to ensure effective stimulation of the mucosal immune system when non-replicating split or subunit antigens were used [11]. A mucosal adjuvant would ideally increase the uptake of the antigen through the mucus and mucous membrane and reduce the required antigen dose while eliciting mucosal as well as systemic immunity. Moreover, the adjuvant should ideally not cause adverse side effects. Concerns about the safety of mucosal adjuvants are real, since the reporting of an increased incidence of Bell’s palsy syndrome seen after using an intranasally administered inactivated influenza vaccine, adjuvanted with an apparently insufficiently detoxified mutant of the E. coli heat labile enterotoxin [12] and [13]. Nevertheless, research on the design and development of effective and safe intranasal adjuvants is ongoing and several mucosal adjuvants which support influenza immunity are currently under investigation [14], [15], [16], [17] and [18].