A Systematic Approach to Understand the Mechanism of Action of the Bisthiazolium Compound T4 on the Human Malaria Parasite, Plasmodium Falciparum

Overview

Journal BMC Genomics

Publisher Biomed Central

Specialty Genetics

Date 2008 Nov 1

PMID 18973684

Citations 40

Authors

Karine G Le Roch

Jeffrey R Johnson

Hugues Ahiboh

Duk-Won D Chung

Jacques Prudhomme

David Plouffe

Kerstin Henson

Yingyao Zhou

William Witola

John R Yates

Choukri Ben Mamoun

Elizabeth A Winzeler

Henri Vial

Affiliations

Soon will be listed here.

Abstract

Background: In recent years, a major increase in the occurrence of drug resistant falciparum malaria has been reported. Choline analogs, such as the bisthiazolium T4, represent a novel class of compounds with strong potency against drug sensitive and resistant P. falciparum clones. Although T4 and its analogs are presumed to target the parasite's lipid metabolism, their exact mechanism of action remains unknown. Here we have employed transcriptome and proteome profiling analyses to characterize the global response of P. falciparum to T4 during the intraerythrocytic cycle of this parasite.

Results: No significant transcriptional changes were detected immediately after addition of T4 despite the drug's effect on the parasite metabolism. Using the Ontology-based Pattern Identification (OPI) algorithm with an increased T4 incubation time, we demonstrated cell cycle arrest and a general induction of genes involved in gametocytogenesis. Proteomic analysis revealed a significant decrease in the level of the choline/ethanolamine-phosphotransferase (PfCEPT), a key enzyme involved in the final step of synthesis of phosphatidylcholine (PC). This effect was further supported by metabolic studies, which showed a major alteration in the synthesis of PC from choline and ethanolamine by the compound.

Conclusion: Our studies demonstrate that the bisthiazolium compound T4 inhibits the pathways of synthesis of phosphatidylcholine from choline and ethanolamine in P. falciparum, and provide evidence for post-transcriptional regulations of parasite metabolism in response to external stimuli.

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