Synthesis, Antimalarial Activity, and Intracellular Targets of MEFAS, a New Hybrid Compound Derived from Mefloquine and Artesunate | Zendy

Fernando de Pilla Varotti | Zendy; Ana Cristina Carvalho Botelho | Zendy; Anderson Assunção Andrade | Zendy; Renata Cristina de Paula | Zendy; Elaine Maria Souza Fagundes | Zendy; Alessandra L. Valverde | Zendy; Lúcia M. U. Mayer | Zendy; Jorge Souza Mendonça | Zendy; M.V.N. De Souza | Zendy; Núbia Boechat | Zendy; Antoniana U. Krettli | Zendy

Open Access

Synthesis, Antimalarial Activity, and Intracellular Targets of MEFAS, a New Hybrid Compound Derived from Mefloquine and Artesunate

Author(s) -

Fernando de Pilla Varotti,

Ana Cristina Carvalho Botelho,

Anderson Assunção Andrade,

Renata Cristina de Paula,

Elaine Maria Souza Fagundes,

Alessandra L. Valverde,

Lúcia M. U. Mayer,

Jorge Souza Mendonça,

M.V.N. De Souza,

Núbia Boechat,

Antoniana U. Krettli

Publication year - 2008

Publication title -

antimicrobial agents and chemotherapy

Language(s) - English

Resource type - Journals

SCImago Journal Rank - 2.07

H-Index - 259

eISSN - 1070-6283

pISSN - 0066-4804

DOI - 10.1128/aac.00510-08

Subject(s) - mefloquine , plasmodium falciparum , chloroquine , parasitemia , pharmacology , hemozoin , artesunate , biology , artemisinin , intracellular , bafilomycin , plasmodium berghei , biochemistry , malaria , immunology , autophagy , apoptosis

A new synthetic antimalarial drug, a salt derived from two antimalarial molecules, mefloquine (MQ) and artesunate (AS), here named MEFAS, has been tested for its pharmacological activity. Combinations of AS plus MQ hydrochloride are currently being used in areas with drug-resistantPlasmodium falciparum parasites; although AS clears parasitemia in shorter time periods than any other antimalarial drug, it does not cure infected patients; in addition, MQ causes side effects and is rather expensive, important problems considering that malaria affects mostly populations in poor countries. Here, we show that MEFAS is more effective than the combination of AS and MQ, tested in parallel at different mass proportions, againstP. falciparum (chloroquine-resistant clone W2 and chloroquine-sensitive clone 3D7) in vitro and in mice infected withPlasmodium berghei , promoting cure of this infection. MEFAS tested against HepG2 hepatoma cells exhibited lower toxicity than the antimalarials AS and MQ alone or combined. Possible targets of MEFAS have been studied by confocal microscopy using fluorescent probes (Fluo-4 AM and BCECF-AM) inP. falciparum synchronous culture of W2-infected red blood cells. Dynamic images show that MEFAS exhibited intracellular action increasing cytoplasmic Ca2+ at 1.0 ng/ml. This effect was also observed in the presence of tapsigargin, an inhibitor of SERCA, suggesting an intracellular target distinct from the endoplasmic reticulum. Trophozoites loaded with BCECF-AM, when treated with MEFAS, were still able to mobilize protons from the digestive vacuole (DV), altering the pH gradient. However, in the presence of bafilomycin A1, an inhibitor of the H+ pump from acidic compartments of eukaryotic cells, MEFAS had no action on the DV. In conclusion, the endoplasmic reticulum and DV are intracellular targets for MEFAS inPlasmodium sp., suggesting two modes of action of this new salt. Our data support MEFAS as a candidate for treating human malaria.

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