Design, Synthesis, and Biological and Crystallographic Evaluation of Novel Inhibitors of Plasmodium Falciparum Enoyl-ACP-reductase (PfFabI)

Overview

Journal J Med Chem

Publisher American Chemical Society

Specialty Chemistry

Date 2013 Sep 26

PMID 24063369

Citations 9

Authors

Federica Belluti

Remo Perozzo

Leonardo Lauciello

Francesco Colizzi

Dirk Kostrewa

Alessandra Bisi

Silvia Gobbi

Angela Rampa

Maria Laura Bolognesi

Maurizio Recanatini

Reto Brun

Leonardo Scapozza

Andrea Cavalli

Affiliations

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Abstract

Malaria, a disease of worldwide significance, is responsible for over one million deaths annually. The liver-stage of Plasmodium's life cycle is the first, obligatory, but clinically silent step in malaria infection. The P. falciparum type II fatty acid biosynthesis pathway (PfFAS-II) has been found to be essential for complete liver-stage development and has been regarded as a potential antimalarial target for the development of drugs for malaria prophylaxis and liver-stage eradication. In this paper, new coumarin-based triclosan analogues are reported and their biological profile is explored in terms of inhibitory potency against enzymes of the PfFAS-II pathway. Among the tested compounds, 7 and 8 showed the highest inhibitory potency against Pf enoyl-ACP-reductase (PfFabI), followed by 15 and 3. Finally, we determined the crystal structures of compounds 7 and 11 in complex with PfFabI to identify their mode of binding and to confirm outcomes of docking simulations.

Citing Articles

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The genome of a Bacteroidetes inhabitant of the human gut encodes a structurally distinct enoyl-acyl carrier protein reductase (FabI).

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