Chemical Genomic Profiling Unveils the in Vitro and in Vivo Antiplasmodial Mechanism of Açaı́ ( Euterpe oleracea Mart.) Polyphenols
Malaria remains a major detrimental parasitic disease in the developing world, with more than 200 million cases annually. Widespread drug-resistant parasite strains push for the development of novel antimalarial drugs. Plant-derived natural products are key sources of antimalarial molecules. Euterpe...
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Veröffentlicht in: | ACS omega 2019-09, Vol.4 (13), p.15628-15635 |
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Sprache: | eng |
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Zusammenfassung: | Malaria remains a
major detrimental parasitic disease in the developing
world, with more than 200 million cases annually. Widespread drug-resistant
parasite strains push for the development of novel antimalarial drugs.
Plant-derived natural products are key sources of antimalarial molecules.
Euterpe oleracea
Martius (“açaí”)
originates from Brazil and has anti-inflammatory and antineoplasic
properties. Here, we evaluated the antimalarial efficacy of three
phenolic fractions of açaí; total phenolics (
1
), nonanthocyanin phenolics (
2
), and total anthocyanins
(
3
). In vitro, fraction
2
moderately inhibited
parasite growth in chloroquine-sensitive (HB3) and multiresistant
(Dd2)
Plasmodium falciparum
strains,
while none of the fractions was toxic to noncancer cells. Despite
the limited activity in vitro, the oral treatment with 20 mg/kg of
fraction
1
reduced parasitemia by 89.4% in
Plasmodium chabaudi
-infected mice and prolonged survival.
Contrasting in vitro and in vivo activities of
1
suggest
key antiplasmodial roles for polyphenol metabolites rather than the
fraction itself. Finally, we performed haploinsufficiency chemical
genomic profiling (HIP) utilizing heterozygous
Saccharomyces
cerevisiae
deletion mutants to identify molecular
mechanisms of açaí fractions. HIP results indicate
proteostasis as the main cellular pathway affected by fraction
2
. These results open avenues to develop açaí
polyphenols as potential new antimalarial candidates. |
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ISSN: | 2470-1343 2470-1343 |
DOI: | 10.1021/acsomega.9b02127 |