Leishmania spp. are medically important intracellular proteozoan parasites. Using a proteomics approach we have previously comprehensively analysed parasite adaptation to its intracellular habitat in macrophages. Here we propose to extend and complement this approach by analysing the host cell-derived membrane and soluble proteins that contribute to this habitat. Specifically we propose to perform a comparative in silico analysis of host phagosomal multiprotein complexes between Leishmania- and latex bead-containing phagosomes to define functionally relevant differences. . Furthermore, we will pursue the relevance of one already identified difference and test the hypothesis that i) Cholesterol/lipid accumulation in Leishmania-PVs, ii) up-regulation of host cell cholesterol synthesis pathways, iii) inhibition of membrane raft dependent signalling cascades and iv) up-regulation of fatty acid catabolism in parasites are mechanistically linked and interdependent. Finally, we simultaneously want to establish experimental platforms based on ES cell- and transgenic mouse-derived primary phagocytic cells that will allow to harness the power of reverse genetics or RNAi to analyse phagosomal protein function in different cell contexts.

DFG Programme Priority Programmes

Subproject of SPP 1580:  Intracellular Compartments as Places of Pathogen-Host Interaction