Identification and characterization of the antiplasmodial activity of Hsp90 inhibitors

Claribel Murillo-Solano; Chunmin Dong; Cecilia G. Sanchez; Juan C. Pizarro

doi:10.1186/s12936-017-1940-7

Malaria Journal (Jul 2017)

Identification and characterization of the antiplasmodial activity of Hsp90 inhibitors

Claribel Murillo-Solano,
Chunmin Dong,
Cecilia G. Sanchez,
Juan C. Pizarro

Affiliations

Claribel Murillo-Solano: Department of Tropical Medicine, School of Public Health and Tropical Medicine, Tulane University
Chunmin Dong: Section of Pulmonary Diseases, Critical Care and Environmental Medicine, Department of Medicine, Tulane University Health Sciences Center
Cecilia G. Sanchez: Section of Pulmonary Diseases, Critical Care and Environmental Medicine, Department of Medicine, Tulane University Health Sciences Center
Juan C. Pizarro: Department of Tropical Medicine, School of Public Health and Tropical Medicine, Tulane University

DOI: https://doi.org/10.1186/s12936-017-1940-7
Journal volume & issue: Vol. 16, no. 1
pp. 1 – 14

Abstract

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Abstract Background The recent reduction in mortality due to malaria is being threatened by the appearance of Plasmodium falciparum parasites that are resistant to artemisinin in Southeast Asia. To limit the impact of resistant parasites and their spread across the world, there is a need to validate anti-malarial drug targets and identify new leads that will serve as foundations for future drug development programmes targeting malaria. Towards that end, the antiplasmodial potential of several Hsp90 inhibitors was characterized. Because, the Hsp90 chaperone has been suggested as a good drug target against multiple parasitic infections including malaria. Results Chemically diverse sets of Hsp90 inhibitors, evaluated in clinical trials as anti-cancer agents, were tested against the malaria parasite. Most of the compounds showed strong antiplasmodial activity in growth inhibition assays against chloroquine sensitive and resistant strains. There was a good agreement between the compound in vitro anti-parasitic activity and their affinity against the Plasmodium chaperone. The two most potent Hsp90 inhibitors also showed cytocidal activity against two P. falciparum strains. Their antiplasmodial activity affected all parasite forms during the malaria blood cycle. However, the compounds activity against the parasite showed no synergy when combined with anti-malarial drugs, like chloroquine or DHA. Discussion The Hsp90 inhibitors anti-parasitic activity correlates with their affinity to their predicted target the P. falciparum chaperone Hsp90. However, the most effective compounds also showed high affinity for a close homologue, Grp94. This association points to a mode of action for Hsp90 inhibitors that correlate compound efficacy with multi-target engagement. Besides their ability to limit parasite replication, two compounds also significantly impacted P. falciparum viability in vitro. Finally, a structural analysis suggests that the best hit represents a promising scaffold to develop parasite specific leads according. Conclusion The results shown that Hsp90 inhibitors are lethal against the malaria parasite. The correlation between biochemical and in vitro data strongly supports Hsp90 as a drug target against the malaria parasite. Furthermore, at least one Hsp90 inhibitor developed as anticancer therapeutics could serve as starting point to generate P. falciparum-specific lead compounds.

Published in Malaria Journal

ISSN: 1475-2875 (Online)
Publisher: BMC
Country of publisher: United Kingdom
LCC subjects: Medicine: Internal medicine: Special situations and conditions: Arctic medicine. Tropical medicine; Medicine: Internal medicine: Infectious and parasitic diseases
Website: https://malariajournal.biomedcentral.com/

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