Studies of the immunogenic and protective properties of third generation vaccines against american tegumentar leishmaniasis

Abstract

The antigens released by parasites are interesting targets for the development of vaccine candidates, since they are one of first molecules to interact with the innate immune system, establishing an intrinsic physiological relationship with host cells. For this reason, these antigens have been target to vaccine development against murine and canine tegumentar and visceral leishmaniosis, respectively. Indeed with the recent publication of Leishmania donovani secretome has become possible develop well-defined vaccine candidates against this tropical disease; however a limiting factor for this purpose is the yield of antigen to further purification. Thus, DNA vaccines become good alternatives to circumvent the problem of protein purification, once target proteins are expressed in vivo. In the present purpose, we will analyze immunogenicity and protective effects of three different DNA vaccines produced from Leishmania (Leishmania) amazonensis genome, using as vector pVAX1 plasmid, which was licensed to human use. BALB/c mice (12 per group) will be immunized with each DNA vaccine, three times at regular intervals of 15 days, intramuscularly, using CpG adjuvant. Following 30 days of last immunization, six animals will be sacrificed and immunological approaches will be performed to analyze the immunogenicity of vaccinations. Other six mice will be subcutaneously challenged in footpad with L. (L.) amazonensis promastigotes. Immunological, functional and histopathological studies will be carried out to analyze the efficacy of vaccines. In addition, heterologous challenges could be performed using L. (Viannia) shawi and L. (V.) braziliensis species. This project aims to contribute for the development of vaccine candidates against American Tegumentar Leishmaniasis. (AU)