Influence of the Plasmodium falciparum P-glycoprotein homologue 1 (pfmdr1 gene product) on the antimalarial action of cyclosporin

doi:10.1093/jac/dkl461

JAC Advance Access originally published online on November 13, 2006
Journal of Antimicrobial Chemotherapy 2007 59(2):197-203; doi:10.1093/jac/dkl461

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© The Author 2006. Published by Oxford University Press on behalf of the British Society for Antimicrobial Chemotherapy. All rights reserved. For Permissions, please e-mail: journals.permissions@oxfordjournals.org

Influence of the Plasmodium falciparum P-glycoprotein homologue 1 (pfmdr1 gene product) on the antimalarial action of cyclosporin

C. S. Gavigan¹^,, M. Shen², S. G. Machado² and A. Bell¹^,*

¹ Department of Microbiology, Moyne Institute of Preventive Medicine, University of Dublin, Trinity College Dublin 2, Ireland ² Office of Biostatistics, US Food and Drug Administration/Center for Drug Evaluation and Research, Silver Spring MD 20993-0002, USA

Received 2 May 2006; returned 1 September 2006; revised 28 September 2006; accepted 19 October 2006

^*Corresponding author. Tel: +353-1-896-1414; Fax: +353-1-679-9294; E-mail: abell{at}tcd.ie

Background and objectives: The immunosuppressant cyclosporinA and a number of other cyclosporins have potent and selectiveantimalarial activity. Their exact mechanism of antimalarialaction is unknown but the structure–activity relationshipsfor malarial parasite inhibition and immunosuppression differmarkedly. The 3'-keto derivative of cyclosporin D (valspodar)is particularly potent against the human malarial parasite Plasmodiumfalciparum in culture but causes negligible immunosuppression.Multidrug resistance in mammalian cancer cells, the result ofoverproduction of the P-glycoprotein, can be reversed by certaincyclosporins, particularly valspodar. We therefore investigatedthe possibility that the antimalarial target of cyclosporinmight be a P-glycoprotein homologue. P. falciparum P-glycoproteinhomologue 1 (Pgh1; the pfmdr1 gene product) is located in thedigestive vacuole (DV) membrane of the parasite. Its functionis unknown but it modulates the susceptibility of parasitesto quinolines and related antimalarial drugs, including quinine,mefloquine, halofantrine and chloroquine, and to artemisinin.

Methods and results: Here we demonstrate that (i) sequence polymorphismsin pfmdr1 altered the susceptibility of parasites to cyclosporinA and (ii) pfmdr1-overexpressing strains were slightly lesssusceptible to the drug. Furthermore, we found synergistic antimalarialinteractions between cyclosporin A and quinine, mefloquine orhalofantrine and antagonism between cyclosporin A and chloroquine.However, we were unable to detect a direct interaction betweencyclosporin and Pgh1.

Conclusions: The amino acid sequence and copy number of Pgh1may influence cyclosporin susceptibility as a result of a directinteraction between the drug and the protein, or via indirecteffects on the physiology of the DV.

Keywords: malaria , cyclosporin A , Pgh1

${dagger}$ Present address. Abbott Ireland Diagnostic Division, FinisklinBusiness Park, Sligo, Ireland.

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