Seasonal influenza is an acute respiratory disease caused by different types of influenza virus which are circulated in all parts of the world. Most people who get influenza can recover from fever and slight symptoms. However, influenza can cause severe illness or even death particularly in newborns, the elderly, and those with underlined disease or without medical treatments. Nowadays, combating the ongoing epidemic influenza is an unmet medical need. Every year the World Health Organization makes predictions on which influenza strains will circulate in the following year so that a vaccine can be designed, manufactured and administered to the public on time. Seasonal influenza vaccines thus designed can protect against specific viral strains but have to be renewed annually to target the upcoming strains, which limits their protective breadth and efficacy. Therefore, developing a universal influenza vaccine which is broadly protective against diverse influenza virus strains would have a great benefit to public health. My research goal is to design a chimeric hemagglutinin (cHA) that contains the head domain from influenza virus B and the stem domain from influenza A to induce broadly protective activity against seasonal influenza and unexpected pandemic influenza. cHA was designed and expressed. The properties of the recombinant protein were further characterized and used for evaluation of the immune response. Moreover, the effects of N-glycosylation on immunogenicity induced by HA nucleoside vaccine were also evaluated. The result showed that cHA protein can elicit significant IgG titer against variants of HA among H1, H3, Vic and Yam and CD8+ and CD4+ T cell response, suggesting that the cHA has the potential to be a universal vaccine.