Abstract EN:

This thesis devoted to visceral leishmaniasis due to L. Infantum, parasitic disease fatal if left untreated, endemic in Mediterranean basin, includes two main parts. We first performed a vaccination trial using cDNA encoding for the L. Infantum protein papLe22 previously described in our laboratory. This highly immunogenic antigen enhances in vitro IL-10 production, cytokine of the Th2 pathway, favoring the development of the infection. After immunization we observed a reorientation of the immune response toward the th1 pattern and a marked decrease of the frequency of parasite circulation. Therefore, papLe22 represents a potential candidate for an antileishmanial vaccine cocktail. The second aprt describes the characterization of a novel L. Infantum protein termed Lepp12. Both recombinant and natural Lepp12 are phosphorylated in vitro by Protein Kinase C (PKC) or PKC-like activities Transfection experiments indicate that Lepp12 specifically enhances basa; and PMA induced IL-1 beta production in myelomonocytic THP-1 cell line. Togethenr these results indicate that in vitre Lepp12 represents a pytative substrate for PKC and enhances the signal transduction pathway involving PKC.