Chemosensitization potential of P-glycoprotein inhibitors in malaria parasites

Laura M Alcantara; Junwon Kim; Carolina B Moraes; Caio H Franco; Kathrin D Franzoi; Sukjun Lee; Lucio H Freitas-Junior; Lawrence S Ayong

doi:10.1016/j.exppara.2013.03.022

Chemosensitization potential of P-glycoprotein inhibitors in malaria parasites

Exp Parasitol. 2013 Jun;134(2):235-43. doi: 10.1016/j.exppara.2013.03.022. Epub 2013 Mar 28.

Authors

Laura M Alcantara¹, Junwon Kim, Carolina B Moraes, Caio H Franco, Kathrin D Franzoi, Sukjun Lee, Lucio H Freitas-Junior, Lawrence S Ayong

Affiliation

¹ Center for Neglected Diseases Drug Discovery, Institut Pasteur Korea, Sampyeong-dong 696, Bundang-gu, Seongnam-si, Gyeonggi-do 463-400, Republic of Korea.

PMID: 23541983
DOI: 10.1016/j.exppara.2013.03.022

Abstract

Members of the ATP-binding cassette (ABC)-type transporter superfamily have been implicated in multidrug resistance in malaria, and various mechanistic models have been postulated to explain their interaction with diverse antimalarial drugs. To gain insight into the pharmacological benefits of inhibiting ABC-type transporters in malaria chemotherapy, we investigated the in vitro chemosensitization potential of various P-glycoprotein inhibitors. A fluorescent chloroquine derivative was synthesized and used to assess the efflux dynamics of chloroquine in MDR and wild type Plasmodium falciparum parasites. This novel BODIPY-based probe accumulated in the digestive vacuole (DV) of CQ-sensitive parasites but less so in MDR cells. Pre-exposure of the MDR parasites to non-cytocidal concentrations of unlabeled chloroquine resulted in a diffused cytoplasmic retention of the probe whereas a similar treatment with the CQR-reversing agent, chlorpheniramine, resulted in DV accumulation. A diffused cytoplasmic distribution of the probe was also obtained following treatment with the P-gp specific inhibitors zosuquidar and tariquidar, whereas treatments with the tyrosine kinase inhibitors gefitinib or imatinib produced a partial accumulation within the DV. Isobologram analyses of the interactions between these inhibitors and the antimalarial drugs chloroquine, mefloquine, and artemisinin revealed distinct patterns of drug synergism, additivity and antagonism. Taken together, the data indicate that competitive tyrosine kinase and noncompetitive P-glycoprotein ATPase-specific inhibitors represent two new classes of chemosensitizing agents in malaria parasites, but caution against the indiscriminate use of these agents in antimalarial drug combinations.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

ATP Binding Cassette Transporter, Subfamily B, Member 1 / antagonists & inhibitors*
Antimalarials / pharmacology*
Artemisinins / pharmacology
Benzamides / pharmacology
Boron Compounds / chemistry
Chloroquine / pharmacology
Chlorpheniramine / pharmacology
Dibenzocycloheptenes / pharmacology
Drug Interactions
Drug Resistance, Multiple
Erythrocytes / parasitology
Fluorescent Dyes / chemistry
Gefitinib
Humans
Imatinib Mesylate
Mefloquine / pharmacology
Piperazines / pharmacology
Plasmodium falciparum / drug effects*
Plasmodium falciparum / metabolism
Protein Kinase Inhibitors / pharmacology
Pyrimidines / pharmacology
Quinazolines / pharmacology
Quinolines / pharmacology

Substances

4,4-difluoro-4-bora-3a,4a-diaza-s-indacene
ATP Binding Cassette Transporter, Subfamily B, Member 1
Antimalarials
Artemisinins
Benzamides
Boron Compounds
Dibenzocycloheptenes
Fluorescent Dyes
Piperazines
Protein Kinase Inhibitors
Pyrimidines
Quinazolines
Quinolines
Chlorpheniramine
zosuquidar trihydrochloride
Chloroquine
Imatinib Mesylate
artemisinin
tariquidar
Gefitinib
Mefloquine