Currently, a challenging goal in the area of cancer treatment is the development of innovative targeted antitumoral immunotherapies with a long-term efficiency. In this context, we took advantage of liposomal nanoparticles properties for the conception of a tunable vaccine platform allowing the strategical conception of vaccines containing: i) a CD4 epitope peptide able to stimulate CD4+ T helper cells ii) a tumor CD8 epitope peptide, which induces the differentiation of CD8+ T cells in cytotoxic T cells and iii) Toll or Nod-Like receptor agonist(s), which act as adjuvant for the activation of dendritic cell. After several screening steps, three vaccines, specific tardeting an orthotopic lung tumor model (TC-1) and differing only by their adjuvant composition, were successfully developed. Subsequently, a comparative study of their efficacy time limit and their immunologic mode of action was performed. This study showed the therapeutic supremacy of liposomal vaccines containing a TLR4 agonist (MPLA). In this work, we demonstrated the value of a customizable liposomal platform for the conception of personalized vaccines and we highlighted the necessity of immune monitoring for a better understanding of vaccines impact and the prediction of their efficacy.