ABSTRACT
Extensive drug resistance in Plasmodium falciparum emphasizes the urgent requirement for novel antimalarial agents. Here we report potent antimalarial activity of a number of diamidine compounds. The lead compound pentamidine is concentrated 500-fold by erythrocytes infected with P. falciparum. Pentamidine accumulation can be blocked by inhibitors of hemoglobin digestion, suggesting that the drug binds to ferriprotoporphyrin IX (FPIX). All of the compounds bound to FPIX in vitro and inhibited the formation of hemozoin. Furthermore, inhibitors of hemoglobin digestion markedly antagonized the antimalarial activity of the diamidines, indicating that binding to FPIX is crucial for the activity of diamidine drugs. Pentamidine was not accumulated into uninfected erythrocytes. Pentamidine transport into infected cells exhibits an initial rapid phase, nonsaturable in the micromolar range and sensitive to inhibition by furosemide and glibenclamide. Changing the counter-ion in the order Cl(-) < Br(-) < NO(2)(-) < I(-) Subject(s)
Erythrocytes/metabolism
, Pentamidine/pharmacokinetics
, Plasmodium falciparum/metabolism
, Trypanocidal Agents/pharmacokinetics
, Animals
, Biological Transport
, Cell Membrane Permeability
, Crystallization
, Drug Delivery Systems
, Drug Design
, Erythrocytes/drug effects
, Erythrocytes/parasitology
, Hemeproteins/drug effects
, Hemin/chemistry
, Hemin/metabolism
, Humans
, In Vitro Techniques
, Models, Molecular
, Parasitic Sensitivity Tests
, Pentamidine/administration & dosage
, Pentamidine/pharmacology
, Plasmodium falciparum/drug effects
, Tritium
, Trypanocidal Agents/administration & dosage
, Trypanocidal Agents/pharmacology
