Artigo

Antiplasmodial activity of synthetic ellipticine derivatives and an isolated analog

Ellipticine has been shown previously to exhibit excellent in vitro antiplasmodial activity and in vivo antimalarial properties that are comparable to those of the control drug chloroquine in a mouse malaria model. Ellipticine derivatives and analogs exhibit antimalarial potential however only a few...

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Autor principal: Montoia, Andréia
Outros Autores: Silva, Luiz Francisco Rocha e, Torres, Zelina Estevam dos Santos, Costa, David Siqueira, Henrique, Marycleuma Campos, Lima, Emerson Silva, Vasconcellos, Marne Carvalho de, Souza, Rita C.Z., Costa, Mônica Regina Farias, Grafov, Andrèi Andriy, Grafova, Iryna A., Eberlin, M. N., Tadei, Wanderli Pedro, Amorim, Rodrigo C.N., Pohlit, Adrian Martin
Grau: Artigo
Idioma: English
Publicado em: Bioorganic and Medicinal Chemistry Letters 2020
Assuntos:
2 Methyl 1,2,3,4 Tetrahydroellipticine
3,4 Dihydroellipticine
7 Nitroellipticine
7,8,9 Tribromoellipticine
7,9 Dibromoellipticine
9 Bromoellipticine
9 Hydroxyellipticine
9 Methoxyellipticine
9 Nitroellipticine
Antimalarial Agent
Chloroquine
Ellipticine
Ellipticine Derivative
Olivacine
Unclassified Drug
Antimalarial Agent
Chloroquine
Ellipticine
Ellipticine Derivative
2 Methyl 1,2,3,4 Tetrahydroellipticine
7 Nitroellipticine
7,9 Dibromoellipticine
9 Nitroellipticine
Antimalarial Agent
Chloroquine
Ellipticine
Ellipticine Derivative
Olivacine
Quinine Sulfate
Antimalarial Activity
Aspidosperma
Aspidosperma Vargasii
Bark
Bromination
Controlled Study
Drug Cytotoxicity
Drug Effect
Drug Isolation
Drug Potency
Fetus
Human
Human Cell
Ic 50
In Vitro Study
Lung Fibroblast
Medicinal Plant
Nitration
Nonhuman
Plasmodium Berghei
Plasmodium Falciparum
Animals
Chemical Structure
Chemistry
Disease Model
Drug Effects
Fibroblast
Mouse
Synthesis
Animals Cell
Animals Experiment
Animals Model
Antiplasmodial Activity
Aspidosperma
Aspidosperma Vargasii
Carbon Nuclear Magnetic Resonance
Drug Structure
Drug Synthesis
Macrophage
Malaria
Malaria Control
Mass Spectrometry
Parasitemia
Proton Nuclear Magnetic Resonance
Aspidosperma
Plasmodium Falciparum
Animal
Antimalarials
Aspidosperma
Chloroquine
Disease Models, Animals
Ellipticines
Fibroblasts
Humans
Mice
Molecular Structure
Plant Bark
Plasmodium Falciparum
Acesso em linha: https://repositorio.inpa.gov.br/handle/1/17604
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spelling oai:repositorio:1-17604 Antiplasmodial activity of synthetic ellipticine derivatives and an isolated analog Montoia, Andréia Silva, Luiz Francisco Rocha e Torres, Zelina Estevam dos Santos Costa, David Siqueira Henrique, Marycleuma Campos Lima, Emerson Silva Vasconcellos, Marne Carvalho de Souza, Rita C.Z. Costa, Mônica Regina Farias Grafov, Andrèi Andriy Grafova, Iryna A. Eberlin, M. N. Tadei, Wanderli Pedro Amorim, Rodrigo C.N. Pohlit, Adrian Martin 2 Methyl 1,2,3,4 Tetrahydroellipticine 3,4 Dihydroellipticine 7 Nitroellipticine 7,8,9 Tribromoellipticine 7,9 Dibromoellipticine 9 Bromoellipticine 9 Hydroxyellipticine 9 Methoxyellipticine 9 Nitroellipticine Antimalarial Agent Chloroquine Ellipticine Ellipticine Derivative Olivacine Unclassified Drug Antimalarial Agent Chloroquine Ellipticine Ellipticine Derivative 2 Methyl 1,2,3,4 Tetrahydroellipticine 7 Nitroellipticine 7,9 Dibromoellipticine 9 Nitroellipticine Antimalarial Agent Chloroquine Ellipticine Ellipticine Derivative Olivacine Quinine Sulfate Antimalarial Activity Aspidosperma Aspidosperma Vargasii Bark Bromination Controlled Study Drug Cytotoxicity Drug Effect Drug Isolation Drug Potency Fetus Human Human Cell Ic 50 In Vitro Study Lung Fibroblast Medicinal Plant Nitration Nonhuman Plasmodium Berghei Plasmodium Falciparum Animals Chemical Structure Chemistry Disease Model Drug Effects Fibroblast Mouse Synthesis Animals Cell Animals Experiment Animals Model Antiplasmodial Activity Aspidosperma Aspidosperma Vargasii Carbon Nuclear Magnetic Resonance Drug Structure Drug Synthesis Macrophage Malaria Malaria Control Mass Spectrometry Parasitemia Proton Nuclear Magnetic Resonance Aspidosperma Plasmodium Falciparum Animal Antimalarials Aspidosperma Chloroquine Disease Models, Animals Ellipticines Fibroblasts Humans Mice Molecular Structure Plant Bark Plasmodium Falciparum Ellipticine has been shown previously to exhibit excellent in vitro antiplasmodial activity and in vivo antimalarial properties that are comparable to those of the control drug chloroquine in a mouse malaria model. Ellipticine derivatives and analogs exhibit antimalarial potential however only a few have been studied to date. Herein, ellipticine and a structural analog were isolated from Aspidosperma vargasii bark. A-ring brominated and nitrated ellipticine derivatives exhibit good in vitro inhibition of Plasmodium falciparum K1 and 3D7 strains. Several of the compounds were found not to be toxic to human fetal lung fibroblasts. 9-Nitroellipticine (IC50 = 0.55 μM) exhibits greater antiplasmodial activity than ellipticine. These results are further evidence of the antimalarial potential of ellipticine derivatives. © 2014 Elsevier Ltd. All rights reserved. 2020-06-15T21:48:29Z 2020-06-15T21:48:29Z 2014 Artigo https://repositorio.inpa.gov.br/handle/1/17604 10.1016/j.bmcl.2014.04.070 en Volume 24, Número 12, Pags. 2631-2634 Restrito Bioorganic and Medicinal Chemistry Letters
institution Instituto Nacional de Pesquisas da Amazônia - Repositório Institucional
collection INPA-RI
language English
topic 2 Methyl 1,2,3,4 Tetrahydroellipticine
3,4 Dihydroellipticine
7 Nitroellipticine
7,8,9 Tribromoellipticine
7,9 Dibromoellipticine
9 Bromoellipticine
9 Hydroxyellipticine
9 Methoxyellipticine
9 Nitroellipticine
Antimalarial Agent
Chloroquine
Ellipticine
Ellipticine Derivative
Olivacine
Unclassified Drug
Antimalarial Agent
Chloroquine
Ellipticine
Ellipticine Derivative
2 Methyl 1,2,3,4 Tetrahydroellipticine
7 Nitroellipticine
7,9 Dibromoellipticine
9 Nitroellipticine
Antimalarial Agent
Chloroquine
Ellipticine
Ellipticine Derivative
Olivacine
Quinine Sulfate
Antimalarial Activity
Aspidosperma
Aspidosperma Vargasii
Bark
Bromination
Controlled Study
Drug Cytotoxicity
Drug Effect
Drug Isolation
Drug Potency
Fetus
Human
Human Cell
Ic 50
In Vitro Study
Lung Fibroblast
Medicinal Plant
Nitration
Nonhuman
Plasmodium Berghei
Plasmodium Falciparum
Animals
Chemical Structure
Chemistry
Disease Model
Drug Effects
Fibroblast
Mouse
Synthesis
Animals Cell
Animals Experiment
Animals Model
Antiplasmodial Activity
Aspidosperma
Aspidosperma Vargasii
Carbon Nuclear Magnetic Resonance
Drug Structure
Drug Synthesis
Macrophage
Malaria
Malaria Control
Mass Spectrometry
Parasitemia
Proton Nuclear Magnetic Resonance
Aspidosperma
Plasmodium Falciparum
Animal
Antimalarials
Aspidosperma
Chloroquine
Disease Models, Animals
Ellipticines
Fibroblasts
Humans
Mice
Molecular Structure
Plant Bark
Plasmodium Falciparum
spellingShingle 2 Methyl 1,2,3,4 Tetrahydroellipticine
3,4 Dihydroellipticine
7 Nitroellipticine
7,8,9 Tribromoellipticine
7,9 Dibromoellipticine
9 Bromoellipticine
9 Hydroxyellipticine
9 Methoxyellipticine
9 Nitroellipticine
Antimalarial Agent
Chloroquine
Ellipticine
Ellipticine Derivative
Olivacine
Unclassified Drug
Antimalarial Agent
Chloroquine
Ellipticine
Ellipticine Derivative
2 Methyl 1,2,3,4 Tetrahydroellipticine
7 Nitroellipticine
7,9 Dibromoellipticine
9 Nitroellipticine
Antimalarial Agent
Chloroquine
Ellipticine
Ellipticine Derivative
Olivacine
Quinine Sulfate
Antimalarial Activity
Aspidosperma
Aspidosperma Vargasii
Bark
Bromination
Controlled Study
Drug Cytotoxicity
Drug Effect
Drug Isolation
Drug Potency
Fetus
Human
Human Cell
Ic 50
In Vitro Study
Lung Fibroblast
Medicinal Plant
Nitration
Nonhuman
Plasmodium Berghei
Plasmodium Falciparum
Animals
Chemical Structure
Chemistry
Disease Model
Drug Effects
Fibroblast
Mouse
Synthesis
Animals Cell
Animals Experiment
Animals Model
Antiplasmodial Activity
Aspidosperma
Aspidosperma Vargasii
Carbon Nuclear Magnetic Resonance
Drug Structure
Drug Synthesis
Macrophage
Malaria
Malaria Control
Mass Spectrometry
Parasitemia
Proton Nuclear Magnetic Resonance
Aspidosperma
Plasmodium Falciparum
Animal
Antimalarials
Aspidosperma
Chloroquine
Disease Models, Animals
Ellipticines
Fibroblasts
Humans
Mice
Molecular Structure
Plant Bark
Plasmodium Falciparum
Montoia, Andréia
Antiplasmodial activity of synthetic ellipticine derivatives and an isolated analog
topic_facet 2 Methyl 1,2,3,4 Tetrahydroellipticine
3,4 Dihydroellipticine
7 Nitroellipticine
7,8,9 Tribromoellipticine
7,9 Dibromoellipticine
9 Bromoellipticine
9 Hydroxyellipticine
9 Methoxyellipticine
9 Nitroellipticine
Antimalarial Agent
Chloroquine
Ellipticine
Ellipticine Derivative
Olivacine
Unclassified Drug
Antimalarial Agent
Chloroquine
Ellipticine
Ellipticine Derivative
2 Methyl 1,2,3,4 Tetrahydroellipticine
7 Nitroellipticine
7,9 Dibromoellipticine
9 Nitroellipticine
Antimalarial Agent
Chloroquine
Ellipticine
Ellipticine Derivative
Olivacine
Quinine Sulfate
Antimalarial Activity
Aspidosperma
Aspidosperma Vargasii
Bark
Bromination
Controlled Study
Drug Cytotoxicity
Drug Effect
Drug Isolation
Drug Potency
Fetus
Human
Human Cell
Ic 50
In Vitro Study
Lung Fibroblast
Medicinal Plant
Nitration
Nonhuman
Plasmodium Berghei
Plasmodium Falciparum
Animals
Chemical Structure
Chemistry
Disease Model
Drug Effects
Fibroblast
Mouse
Synthesis
Animals Cell
Animals Experiment
Animals Model
Antiplasmodial Activity
Aspidosperma
Aspidosperma Vargasii
Carbon Nuclear Magnetic Resonance
Drug Structure
Drug Synthesis
Macrophage
Malaria
Malaria Control
Mass Spectrometry
Parasitemia
Proton Nuclear Magnetic Resonance
Aspidosperma
Plasmodium Falciparum
Animal
Antimalarials
Aspidosperma
Chloroquine
Disease Models, Animals
Ellipticines
Fibroblasts
Humans
Mice
Molecular Structure
Plant Bark
Plasmodium Falciparum
description Ellipticine has been shown previously to exhibit excellent in vitro antiplasmodial activity and in vivo antimalarial properties that are comparable to those of the control drug chloroquine in a mouse malaria model. Ellipticine derivatives and analogs exhibit antimalarial potential however only a few have been studied to date. Herein, ellipticine and a structural analog were isolated from Aspidosperma vargasii bark. A-ring brominated and nitrated ellipticine derivatives exhibit good in vitro inhibition of Plasmodium falciparum K1 and 3D7 strains. Several of the compounds were found not to be toxic to human fetal lung fibroblasts. 9-Nitroellipticine (IC50 = 0.55 μM) exhibits greater antiplasmodial activity than ellipticine. These results are further evidence of the antimalarial potential of ellipticine derivatives. © 2014 Elsevier Ltd. All rights reserved.
format Artigo
author Montoia, Andréia
author2 Silva, Luiz Francisco Rocha e
Torres, Zelina Estevam dos Santos
Costa, David Siqueira
Henrique, Marycleuma Campos
Lima, Emerson Silva
Vasconcellos, Marne Carvalho de
Souza, Rita C.Z.
Costa, Mônica Regina Farias
Grafov, Andrèi Andriy
Grafova, Iryna A.
Eberlin, M. N.
Tadei, Wanderli Pedro
Amorim, Rodrigo C.N.
Pohlit, Adrian Martin
author2Str Silva, Luiz Francisco Rocha e
Torres, Zelina Estevam dos Santos
Costa, David Siqueira
Henrique, Marycleuma Campos
Lima, Emerson Silva
Vasconcellos, Marne Carvalho de
Souza, Rita C.Z.
Costa, Mônica Regina Farias
Grafov, Andrèi Andriy
Grafova, Iryna A.
Eberlin, M. N.
Tadei, Wanderli Pedro
Amorim, Rodrigo C.N.
Pohlit, Adrian Martin
title Antiplasmodial activity of synthetic ellipticine derivatives and an isolated analog
title_short Antiplasmodial activity of synthetic ellipticine derivatives and an isolated analog
title_full Antiplasmodial activity of synthetic ellipticine derivatives and an isolated analog
title_fullStr Antiplasmodial activity of synthetic ellipticine derivatives and an isolated analog
title_full_unstemmed Antiplasmodial activity of synthetic ellipticine derivatives and an isolated analog
title_sort antiplasmodial activity of synthetic ellipticine derivatives and an isolated analog
publisher Bioorganic and Medicinal Chemistry Letters
publishDate 2020
url https://repositorio.inpa.gov.br/handle/1/17604
_version_ 1787141487284191232
score 11.755432

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