| Literature DB >> 27439976 |
Taís S Macedo1, Legna Colina-Vegas2, Marcelo DA Paixão1, Maribel Navarro3, Breno C Barreto1, Poliana C M Oliveira1, Simone G Macambira4, Marta Machado5, Miguel Prudêncio5, Sarah D'Alessandro6, Nicoletta Basilico7, Diogo R M Moreira1, Alzir A Batista2, Milena B P Soares1.
Abstract
We report the pharmacological activity of organoruthenium complexes containing chloroquine (CQ) as a chelating ligand. The complexes displayed intraerythrocytic activity against CQ-sensitive 3D7 and CQ-resistant W2 strains of Plasmodium falciparum, with potency and selectivity indexes similar to those of CQ. Complexes displayed activity against all intraerythrocytic stages, but moderate activity against Plasmodium berghei liver stages. However, unlike CQ, organoruthenium complexes impaired gametocyte viability and exhibited fast parasiticidal activity against trophozoites for P. falciparum. This functional property results from the ability of complexes to quickly induce oxidative stress. The parasitaemia of P. berghei-infected mice was reduced by treatment with the complex. Our findings demonstrated that using chloroquine for the synthesis of organoruthenium complexes retains potency and selectivity while leading to an increase in the spectrum of action and parasite killing rate relative to CQ.Entities:
Keywords: Malaria; Plasmodium berghei; Plasmodium falciparum; chloroquine; organoruthenium complexes; oxidative stress
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Year: 2016 PMID: 27439976 DOI: 10.1017/S0031182016001153
Source DB: PubMed Journal: Parasitology ISSN: 0031-1820 Impact factor: 3.234