Malaria remains a global public health problem and worsening with the resistance of Plasmodium falciparum to Artemisinin-based Combination Therapies (ACTs), the latest and most effective antimalarial drugs. My project aimed to provide insight into malaria elimination in Indonesia. The first part was to look for new antimalarial drugs based on Indonesian ethnobotanical data. Among 25 crude extracts realized on Indonesian traditional medicinal plants, seven showed a good antimalarial activity (IC50 < 5µg/mL) and some of them were also active against Babesia divergens and Leishmania infantum. The second part of the study focused on chemosynthetic organometallic compounds. The structure- activity relationships study on organometallic gold(I)-NHC complexes led to a very active compound on P. falciparum with an IC50 of 320nM. The third part of this work was dedicated to the study of P. falciparum resistance to artemisinin and its derivatives. The correlation between PfK13 polymorphism and artemisinin resistance has been clearly established thanks to reverse genetic with resistant and sensitive laboratory strains and clinical isolates from Cambodia. This resistance was evidenced in vitro throughout a parasite survival assay called RSA(0-3h). By the same genotypic and phenotypic methods, mapping of PfK13 polymorphism distribution in Indonesia was performed in Kupang on P. falciparum malaria patients. However, at the time of P. falciparum blood samples collection, prevalence showed a dramatic decrease hindering the continuation of the clinical study. Facing to the very small number of eligible patients with a P. falciparum malaria, no conclusive results has been obtained. In conclusion, medicinal plants and synthetic compounds are potentially interesting as chemical starting point for new antimalarial drugs. Concerning artemisinin resistance, any treatment failure or delayed cure with ACTs has yet to be reported in Indonesia. However, because Indonesia is relatively close to the Southeast Asian areas of resistance, the possible occurrence of such cases in Indonesia must be anticipated by determining the variations of P. falciparum malaria chemo-sensitivity and by following PfK13 polymorphism, responsible for artemisinin resistance.