Evaluation of Antimalarial Activity and Toxicity of a New Primaquine Prodrug

Davanço, Marcelo Gomes; Aguiar, Anna Caroline Campos; Santos, Leandro Alves dos; Padilha, Elias Carvalho; Campos, Marcelo Lattarulo; Andrade, Cléverton Roberto de; Fonseca, Luiz Marcos da; Santos, Jean Leandro dos; Chin, Chung Man; Krettli, Antoniana U.; Peccinini, Rosângela Gonçalves

doi:10.1371/journal.pone.0105217

Cited by 18 publications

(15 citation statements)

References 45 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…); (iii) incubation time (30 min (Hollmann et al 2016;Wu et al 2014), 1 hour (Chongsiriwatana et al 2008;Dennison and Phoenix 2014;Yang et al 2013), 4 hrs (Li et al 2005) or 18-24 hrs (Mojsoska et al 2015)); (iii) used positive control (0.1% Triton-X (Dennison and Phoenix 2014;Lee and Lee 2008;Song et al 2005), 1% Triton-X (Mojsoska et al 2015), 10% Triton-X (Wu et al 2014), distilled water (Hollmann et al 2016;Yang et al 2013), 2 % SDS (Zeitler et al 2013), 0.05% saponin (Davanco et al 2014). There are differences even in the used wavelength at which the optical density of released haemoglobin is determined (λ=350 nm (Chongsiriwatana et al 2008), 405-415 nm (Kaushik et al 2012;Lee and Lee 2008;Song et al 2005;Zeitler et al 2013) , 540-550 nm (Davanco et al 2014;Hollmann et al 2016;Mojsoska et al 2015;Yang et al 2013) or 570 nm (Dennison and Phoenix 2014;Wu et al 2014)). …”

Section: Experimental Conditions Of In Vitro Assaysmentioning

confidence: 99%

Comparative analysis of internalisation, haemolytic, cytotoxic and antibacterial effect of membrane-active cationic peptides: aspects of experimental setup

et al. 2017

View full text Add to dashboard Cite

Comparative analysis of internalisation, haemolytic, cytotoxic and antibacterial effect of membrane-active cationic peptides: aspects of experimental setup.Horváti K, Bacsa B, Mlinkó T, Szabó N, Hudecz F, Zsila F, Bősze S. The most selective peptide was the Penetratin, where the effective antimicrobial concentration on pneumococcus was more than 250-times lower than the HC50 value. Therefore, these peptides and their analogues will be further investigated as drug delivery systems for antimicrobial agents.

show abstract

Section: Experimental Conditions Of In Vitro Assaysmentioning

confidence: 99%

Comparative analysis of internalisation, haemolytic, cytotoxic and antibacterial effect of membrane-active cationic peptides: aspects of experimental setup

et al. 2017

View full text Add to dashboard Cite

show abstract

“…However, it has hemolytic effects, especially in people with glucose-6-phosphate dehydrogenase deficiency (G6PD), in which primaquine as a stressor to the erythrocyte induces hemolysis. Hemolysis induced by primaquine can result in discoloration of urine and faeces and it is dose related [ 8 , 9 ]. Gastrointestinal disorders, such as nausea, dizziness, and vomiting, are common but usually not present as severe complications, especially when primaquine is administered with food.…”

Section: Introductionmentioning

confidence: 99%

Side Effects of Chloroquine and Primaquine and Symptom Reduction in Malaria Endemic Area (Mâncio Lima, Acre, Brazil)

Braga

Martins

Cayotopa

et al. 2015

Interdisciplinary Perspectives on Infectious Diseases

View full text Add to dashboard Cite

Side effects of antimalarial drug can overlap with malaria symptoms. We evaluated 50 patients with vivax malaria in Mâncio Lima, Acre, treated with chloroquine and primaquine. Patients were evaluated for the presence of 21 symptoms before and after treatment and for reported side effects of these drugs after treatment was started. The most frequent symptoms before medication were headache, fever, chills, sweating, arthralgia, back pain, and weakness, which were present in between 40% and 76% of respondents. The treatment reduced the occurrence of these symptoms and reduced the lack of appetite, but gastrointestinal symptoms and choluria increased in frequency. There were no reports of pale stools before medication, but 12% reported the occurrence of this symptom after treatment started. Other symptoms such as blurred vision (54%), pruritus (22%), paresthesia (6%), insomnia (46%), and “stings” into the skin (22%) were reported after chloroquine was taken. The antimalarial drugs used to treat P. vivax malaria reduce much of the systemic and algic symptoms but cause mainly gastrointestinal side effects that may lead to lack of adherence to drug treatment. It is important to guide the patient for the appearance and the transience of such side effects in order to avoid abandoning treatment.

show abstract

“…The naphthoquinone derivatives are toxic and several studies have shown that the structure changes in the molecule have reduced its cytotoxic effect, and improve biological activity. Davanço et al [9] , evaluated a prodrug primaquine and when compared with the primaquine, it was less cytotoxic to BGM and HepG2 cells, caused less hemolysis of G6PD deficient red blood cells and caused less alteration in the biochemical parameters. In their study Oliveira et al [31] produced a derivative of vanillin molecule from its condensation with resorcinol and absence of cytotoxicity observed in murine macrophage cells derived compound, while the vanillin presented an IC50 of 645 μg/mL.…”

Section: Discussionmentioning

confidence: 99%

Cytotoxicity, hemolysis and in vivo acute toxicity of 2-hydroxy-3-anilino-1,4-naphthoquinone derivatives

et al. 2016

View full text Add to dashboard Cite

The 1,4-naphthoquinones, important members of the family of quinones are used as both crude extracts and as compound manipulated by the pharmaceutical industry. They have gained great emphasis by presenting different pharmacological properties as antibacterial, antiviral, antiprotozoal and anthelmintic, and has antitumor activity. Our aim was to evaluate the cytotoxicity, hemolytic activity and in vivo acute toxicity of three derivatives of 2-hydroxy-1,4-naphthoquinones. The cell viability in vitro against RAW Cell Line displayed IC50 ranging of 483.5–2044.8 μM, whereas in primary culture tests using murine macrophages, IC50 were 315.8–1408.0 μM for naphthoquinones derivatives 4a and 4c respectively, besides no hemolysis was observed at the dose tested. The in vivo acute toxicity assays exhibited a significant safety margin indicated by a lack of systemic and behavioral toxicity up to 300 mg/kg, and at a dose of 1000 mg/kg the derivatives not triggering signs of toxicity although the compound 4a have promoted hepatic steatosis and hyperemia in kidney tissue. Thereby, these modifications decrease the toxicity of the tested derivatives naphthoquinones, providing a high potential for the development of news drugs.

show abstract

Evaluation of Antimalarial Activity and Toxicity of a New Primaquine Prodrug

Cited by 18 publications

References 45 publications

Comparative analysis of internalisation, haemolytic, cytotoxic and antibacterial effect of membrane-active cationic peptides: aspects of experimental setup

Comparative analysis of internalisation, haemolytic, cytotoxic and antibacterial effect of membrane-active cationic peptides: aspects of experimental setup

Side Effects of Chloroquine and Primaquine and Symptom Reduction in Malaria Endemic Area (Mâncio Lima, Acre, Brazil)

Cytotoxicity, hemolysis and in vivo acute toxicity of 2-hydroxy-3-anilino-1,4-naphthoquinone derivatives

Contact Info

Product

Resources

About