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Use este identificador para citar ou linkar para este item: https://repositorio.inpa.gov.br/handle/1/17457
Título: In vivo evaluation of isolated triterpenes and semi-synthetic derivatives as antimalarial agents
Autor: Silva, Luiz Francisco Rocha e
Ramalhete, Cátia
Nogueira, Karla Lagos
Mulhovo, Silva
Ferreira, Maria José Umbelino
Pohlit, Adrian Martin
Palavras-chave: Antimalarial Agent
Balsaminoside B
Chloroquine
Karavilagenin C
Karavoate B
Karavoate D
Plant Extract
Triterpene
Unclassified Drug
Antimalarial Agent
Triterpene
African Medicine
Animals Experiment
Animals Model
Antimalarial Activity
Carbon Nuclear Magnetic Resonance
Chemical Structure
Controlled Study
Cytotoxicity
Drug Isolation
Female
High Performance Liquid Chromatography
Human
Human Cell
Ic 50
In Vitro Study
In Vivo Study
Malaria
Mass Spectrometry
Mcf 7 Cell Line
Momordica Balsamina
Mouse
Nonhuman
Parasitemia
Phytochemistry
Plasmodium Berghei
Plasmodium Falciparum
Proton Nuclear Magnetic Resonance
Structure Activity Relation
Survival Time
Treatment Outcome
Chemistry
Dose Response
Drug Effects
Drug Sensitivity
Isolation And Purification
Malaria
Momordica
Parasitology
Antimalarials
Dose-response Relationship, Drug
Malaria
Molecular Structure
Momordica
Parasitic Sensitivity Tests
Plasmodium Falciparum
Structure-activity Relationship
Triterpenes
Data do documento: 2015
Revista: European Journal of Medicinal Chemistry
É parte de: Volume 102, Pags. 398-402
Abstract: The triterpenes balsaminoside B (1) and karavilagenin C (2) were isolated from the African medicinal plant Momordica balsamina L. Karavoates B (3) and D (4) were synthesized by diacylation of 2 with acetic and propionic anhydrides, respectively. In previous work, derivatives 3 and 4 exhibited submicromolar median inhibitory concentrations (IC<inf>50</inf>) in vitro against Plasmodium falciparum Welch (human malaria parasite) strains 20 to 25 times lower than those of natural product 2. The main objective of the present study was to explore structure-in vivo antimalarial activity relationships (SAR) for compounds 1-4 in Plasmodium berghei Vincke and Lips NK65-infected mice in the 4 day suppressive test. Semi-synthetic derivatives 3 and 4 exhibited greater in vivo antimalarial activity than isolates 1 and 2. Orally and subcutaneously administered karavoate B exhibited the greatest in vivo antimalarial activity (55.2-58.1% maximal suppression of parasitemia at doses of 50 mg kg-1 day-1). Diacylation of natural isolate 2 with short chain carboxylic acid moieties yielded derivatives with enhanced maximal in vivo parasitemia suppression for both routes of administration. Maximal in vivo parasite suppression by diacetyl derivative 3 was roughly double that of natural precursor 2. © 2015 Published by Elsevier Masson SAS.
DOI: 10.1016/j.ejmech.2015.08.022
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