| Literature DB >> 26472355 |
Nathalie Bürstner1, Silvio Roggo1, Nils Ostermann1, Jutta Blank1, Cecile Delmas1, Felix Freuler1, Bernd Gerhartz1, Alexandra Hinniger1, Dominic Hoepfner1, Brigitta Liechty1, Manuel Mihalic1, Jason Murphy2, Dominik Pistorius1, Matthias Rottmann3, Jason R Thomas2, Markus Schirle2, Esther K Schmitt4.
Abstract
Malaria continues to be one of the most devastating human diseases despite many efforts to limit its spread by prevention of infection or by pharmaceutical treatment of patients. We have conducted a screen for antiplasmodial compounds by using a natural product library. Here we report on cyclomarin A as a potent growth inhibitor of Plasmodium falciparum and the identification of its molecular target, diadenosine triphosphate hydrolase (PfAp3Aase), by chemical proteomics. Using a biochemical assay, we could show that cyclomarin A is a specific inhibitor of the plasmodial enzyme but not of the closest human homologue hFHIT. Co-crystallisation experiments demonstrate a unique binding mode of the inhibitor. One molecule of cyclomarin A binds a dimeric PfAp3Aase and prevents the formation of the enzyme⋅substrate complex. These results validate PfAp3Aase as a new drug target for the treatment of malaria. We have previously elucidated the structurally unrelated regulatory subunit ClpC1 of the ClpP protease as the molecular target of cyclomarin A in Mycobacterium tuberculosis. Thus, cyclomarin A is a rare example of a natural product with two distinct and specific modes of action.Entities:
Keywords: antiprotozoal agents; cyclomarin; diadenosine triphosphate; malaria; natural products
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Year: 2015 PMID: 26472355 DOI: 10.1002/cbic.201500472
Source DB: PubMed Journal: Chembiochem ISSN: 1439-4227 Impact factor: 3.164