Abstract EN:

This thesis is focused on the asymmetric synthesis and the study of the reactivity of a trifluoromethyl alpha amino epoxide, and the synthesis of a CF3-analogue of a known plasmepsin II inhibitor. Plasmepsin II is an aspartyl protease specific of Plasmodium, the parasite responsible of malaria. Due to increasing resistance of the parasite to the current antimalarial treatments, plasmepsins are becoming preferential targets for new therapies. The diaminoalcohol scaffold present on the inhibitors of this protease is easily obtained by the ring opening of an alpha-aminoepoxide. Some previous works lead us to the synthesis of a CF3-analogue of this epoxide. We first studied thereactivity of this analogue towards nitrogenous reagents in order to consider new structural units of plasmepsin II inhibitors. This study was completed by the investigationof a new access to the two enantiomers of the CF3-epoxide. Finally, a total synthesis of a CF3-analogue of an inhibitor known in the literature was described. In the last part, we investigated the stereoselective synthesis of beta-aminoesters by a new insight into the Reformatsky reaction. We have also performed the synthesis of alpha-trifluoromethyl aliphatic amines by addition of organozinc reagents.