Blood shizonticidal activities of phenazines and naphthoquinoidal compounds against Plasmodium falciparum in vitro and in mice malaria studies

Souza, Nicolli Bellotti de; Andrade, Isabel M de; Carneiro, Paula F.; Jardim, Guilherme A. M.; Melo, Isadora M.M. de; Júnior, Eufrânio N. da Silva; Krettli, Antoniana U.

doi:10.1590/0074-0276130603

Cited by 24 publications

(6 citation statements)

References 47 publications

(55 reference statements)

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“…The compounds obtained by our new method are structurally similar to the naphthoquinones that we, and others, have synthesized and evaluated during the last few years against clinical targets, such as cancer, malaria, leishmania and tuberculosis, i.e. diseases with an inherently disturbed intracellular redox‐balance.…”

Section: Resultsmentioning

confidence: 93%

Ruthenium(II)‐Catalyzed C–H Alkenylation of Quinones: Diversity‐Oriented Strategy for Trypanocidal Compounds

et al. 2019

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Ruthenium(II)‐catalysis enabled C–H alkenylations of unactivated naphthoquinones for the preparation of A‐ring‐modified naphthoquinoidal compounds with activity against Trypanosoma cruzi, the parasite causing Chagas disease. The present study encompasses C–H alkenylation by weak O‐coordination by means of ruthenium(II) carboxylates. This method provided an efficient and versatile tool towards a diversity‐oriented strategy for the preparation of compounds with a relevant biological profile.

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Section: Resultsmentioning

confidence: 93%

Ruthenium(II)‐Catalyzed C–H Alkenylation of Quinones: Diversity‐Oriented Strategy for Trypanocidal Compounds

et al. 2019

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“…The percentage inhibition of parasite multiplication was calculated comparing the treated group with untreated group by means of the following formula 39 [(A − B)/A] × 100; where A = parasitaemia in the untreated group and B = parasitemia in the test group. Compounds that reduced parasitemia by 40% were considered active, whereas those that reduce parasitaemia by 30–40% or less than 30% were deemed partially active and inactive, respectively 40 . Most of the compounds were active against P. berghei after 7 days post-infection by reducing the parasiteamia by at least 40% when in a dose of 100 mg/kg (Table 5).…”

Section: Resultsmentioning

confidence: 99%

New peptide derived antimalaria and antimicrobial agents bearing sulphonamide moiety

Ugwuja

Okoro

Soman

et al. 2019

Journal of Enzyme Inhibition and Medicinal Chemistry

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Fourteen novel dipeptide carboxamide derivatives bearing benzensulphonamoyl propanamide were synthesized and characterized using 1 H NMR, 13 C NMR, FTIR and MS spectroscopic techniques. In vivo antimalarial and in vitro antimicrobial studies were carried out on these synthesized compounds. Molecular docking, haematological analysis, liver and kidney function tests were also evaluated to assess the effect of the compounds on the organs. At 200 mg/kg body weight, 7i inhibited the multiplication of the parasite by 81.38% on day 12 of post-treatment exposure. This was comparable to the 82.34% reduction with artemisinin. The minimum inhibitory concentration (MIC) in µM ranged from 0.03 to 2.34 with 7h having MIC of 0.03 µM against Plasmodium falciparium. The in vitro antibacterial activity of the compounds against some clinically isolated bacteria strains showed varied activities with some of the new compounds showing better activities against the bacteria and the fungi more than the reference drug ciprofloxacin and fluconazole.

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“…The phenylpiperazine is attached to a piperazine phenylaniline, showing similarity with radicals used in structural changes, as in the present study, which is aniline derivatives and associated with the effectiveness of that radical. In another study, eight derivatives of 2-hydroxy-3-methylamino-1.4-naphthoquinone were tested, and five were active, exhibiting IC 50 values less than 30 μM against P. falciparum W2 (chloroquine-resistant strain) [10].…”

Section: Discussionmentioning

confidence: 99%

“…The antiparasitic activity of hydroxy-naphthoquinones derivatives is already known, with studies confirming its efficacy against Leishmania braziliensis and Leishmania amazonensis [4], Trypanosoma cruzi [5] and P. falciparum [6–10]. Its mechanism of action was already proposed by means of the inhibition of the mitochondrial electron carrier chain [11].…”

Section: Introductionmentioning

confidence: 99%

In vitro antiplasmodial activity, pharmacokinetic profiles and interference in isoprenoid pathway of 2-aniline-3-hydroxy-1.4-naphthoquinone derivatives

Pereira

Emery

Lobo

et al. 2018

Malar J

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BackgroundPlasmodium falciparum has shown multidrug resistance, leading to the necessity for the development of new drugs with novel targets, such as the synthesis of isoprenic precursors, which are excellent targets because the pathway is different in several steps when compared with the human host. Naphthoquinone derivatives have been described as potentially promising for the development of anti-malarial leader molecules. In view of that, the focus in this work is twofold: first, evaluate the in vitro naphthoquinone antiplasmodial activity and cytotoxicity; secondly, investigate one possible action mechanism of two derivatives of hydroxy-naphthoquinones.ResultsThe two hydroxy-naphthoquinones derivatives have been tested against P. falciparum in vitro, using strains of parasites chloroquine-sensitive (3D7) and chloroquine-resistant (Dd2), causing 50% inhibition of parasite growth with concentrations that varied from 7 to 44.5 μM. The cell viability in vitro against RAW Cell Line displayed IC50 = 483.5 and 714.9 μM, whereas, in primary culture tests using murine macrophages, IC50 were 315.8 and 532.6 μM for the two selected compounds, causing no haemolysis at the doses tested. The in vivo acute toxicity assays exhibited a significant safety margin indicated by a lack of systemic and behavioural toxicity up to 300 mg/kg. It is suggested that this drug seems to inhibit the biosynthesis of isoprenic compounds, particularly the menaquinone and tocopherol.ConclusionsThese derivatives have a high potential for the development of new anti-malarial drugs since they showed low toxicity associated to a satisfactory antiplasmodial activity and possible inhibition of a metabolic pathway distinct from the pathways found in the mammalian host.

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Blood shizonticidal activities of phenazines and naphthoquinoidal compounds against Plasmodium falciparum in vitro and in mice malaria studies

Cited by 24 publications

References 47 publications

Ruthenium(II)‐Catalyzed C–H Alkenylation of Quinones: Diversity‐Oriented Strategy for Trypanocidal Compounds

Ruthenium(II)‐Catalyzed C–H Alkenylation of Quinones: Diversity‐Oriented Strategy for Trypanocidal Compounds

New peptide derived antimalaria and antimicrobial agents bearing sulphonamide moiety

In vitro antiplasmodial activity, pharmacokinetic profiles and interference in isoprenoid pathway of 2-aniline-3-hydroxy-1.4-naphthoquinone derivatives

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