The Immunology of Leishmania Infection and the Implications for Vaccine Development

doi:10.1196/annals.1307.041

Leishmania parasites are vector-borne protozoal pathogens foundin tropical and subtropical regions of both the Old and NewWorld. These parasites can cause visceral or cutaneous disease,and the pathology of the infection is determined by both hostimmune factors and species/strain differences of the parasite.Dogs are an important reservoir for maintaining the populationof Leishmania parasites that can lead to visceral leishmaniasisin humans, and a vaccination approach may be an effective methodfor reducing the numbers of infected dogs. Resistance to leishmaniasishas been consistently associated with a T helper 1 immune response,characterized by the production of IFN-gamma by the antigen-specificlymphocyte population. The development of this Th1 responsehas been shown to be dependent upon both cytokines and dendriticcells during T cell activation. However, the development ofa Leishmania vaccine effective in preventing these chronic diseaseshas proven to be a challenge. Vaccine trials have focused onwhole-killed or subunit vaccines with adjuvants. Newer experimentalstrategies involve the attenuation of the Leishmania parasitevia gene deletion technologies or the expression of specificLeishmania peptides within attenuated organisms, such as BacillusCalmette Guérin. DNA vaccines and dendritic cell potentiators,such as CpG oligodeoxynucleotides and Flt-3 ligand, are alsoin the early stage of development. In addition, as part of blockingthe transmission cycle of leishmaniasis, several laboratoriesare also exploring the possibility of immunomodulating the hosttoward the bite of the sand fly.