Abstract

Ethnopharmacological relevanceFrom seeds of Carapa guianensis the Amazon native people extracts the andiroba oil, which is traditionally used as febrifuge, anti-malarial, insecticidal and repellant. The non-saponifiable fraction separated from the oil is rich in limonoids, which assigns its pharmacological effects. Materials and methodsThe andiroba oil and its limonoid-rich fraction were submitted to in vitro antiplasmodial bioassay using W2 and Dd2 strains of Plasmodium falciparum. The acute toxicity of andiroba oil was evaluated. The limonoid-rich fraction was subjected to fractionation and identified its major constituents. ResultsAndiroba oil and its limonoid-rich fraction inhibited the growth of W2 clone in 100%, between 24 and 72h, at concentrations of 8.2μg/mL and 3.1μg/mL, respectively. Under the same conditions, the parasitaemia of Dd2 clone provoked by the andiroba oil showed inhibition of 31% (IC50 >82μg/mL) with a time-dependent relationship of 24h and inhibition of 88% (IC50 8.4μg/mL) after 72h, while for the limonoid-rich fraction the inhibition of Dd2 clone was 56% (IC50 2.8μg/mL) at 24h and 82% (IC50 0.4μg/mL) after 72h. Andiroba oil in acute toxicity test with a fixed dose (LD50 >2000mg/kg) was not toxic The limonoids identified in the oil were gedunin, 6α-acetoxygedunin, 7-deacetoxy-7-oxogedunin, 7-deacetylgedunin, 1,2-dihydro-3β-hydroxy-7-deacetoxy-7-oxogedunin and andirobin. Gedunin and derivatives has been reputed as anti-malarials. ConclusionThe results support the traditional use of andiroba oil as antiplasmodial, which additionally proved not to be toxic in bioassays conducted with mice.

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