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A type II pathway for fatty acid biosynthesis presents drug targets in Plasmodium falciparum.


ABSTRACT: It has long been held that the malaria parasite, Plasmodium sp., is incapable of de novo fatty acid synthesis. This view has recently been overturned with the emergence of data for the presence of a fatty acid biosynthetic pathway in the relict plastid of P. falciparum (known as the apicoplast). This pathway represents the type II pathway common to plant chloroplasts and bacteria but distinct from the type I pathway of animals including humans. Specific inhibitors of the type II pathway, thiolactomycin and triclosan, have been reported to target this Plasmodium pathway. Here we report further inhibitors of the plastid-based pathway that inhibit Plasmodium parasites. These include several analogues of thiolactomycin, two with sixfold-greater efficacy than thiolactomycin. We also report that parasites respond very rapidly to such inhibitors and that the greatest sensitivity is seen in ring-stage parasites. This study substantiates the importance of fatty acid synthesis for blood-stage parasite survival and shows that this pathway provides scope for the development of novel antimalarial drugs.

SUBMITTER: Waller RF 

PROVIDER: S-EPMC148988 | biostudies-literature | 2003 Jan

REPOSITORIES: biostudies-literature

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A type II pathway for fatty acid biosynthesis presents drug targets in Plasmodium falciparum.

Waller Ross F RF   Ralph Stuart A SA   Reed Michael B MB   Su Vanessa V   Douglas James D JD   Minnikin David E DE   Cowman Alan F AF   Besra Gurdyal S GS   McFadden Geoffrey I GI  

Antimicrobial agents and chemotherapy 20030101 1


It has long been held that the malaria parasite, Plasmodium sp., is incapable of de novo fatty acid synthesis. This view has recently been overturned with the emergence of data for the presence of a fatty acid biosynthetic pathway in the relict plastid of P. falciparum (known as the apicoplast). This pathway represents the type II pathway common to plant chloroplasts and bacteria but distinct from the type I pathway of animals including humans. Specific inhibitors of the type II pathway, thiolac  ...[more]

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