Significant progress in evaluation of host parasite interactions in the Plasmodium berghei model has been achieved with GFP or luciferase transgenic parasites. Although Plasmodium chabaudi is considered to be a much better model for Plasmodium falciparum than P. berghei, methods for manipulation of the P. chabaudi genome are hitherto not available. The aim of this application is to establish GFP-luciferase transgenic P. chabaudi. These parasites will then be used to analyze effects of exclusion of parasitized erythrocytes from the spleen (spleen ‘closing’) in wild-type but not lymphotoxin β receptor-deficient (LTβR-/-) mice on parasite sequestration and their interaction with phagocytic cells. The transgenic parasites will also be used to select antigenically new parasite variants by passage through wild-type or LTβR-/- mice. These experiments will reveal if spleen passage exerts a selective immune pressure on the parasite and if immune evasion by antigenic variation counteracts this pressure. Moreover, the results will show whether antigenically different parasites exhibit different sequestration patterns.

DFG-Verfahren Sachbeihilfen

Ehemalige Antragstellerin Professorin Dr. Janina Demeler, bis 10/2009