Pyrazoleamide compounds are potent antimalarials that target Na+ homeostasis in intraerythrocytic Plasmodium falciparum

Akhil B Vaidya; Joanne M Morrisey; Zhongsheng Zhang; Sudipta Das; Thomas M Daly; Thomas D Otto; Natalie J Spillman; Matthew Wyvratt; Peter Siegl; Jutta Marfurt; Grennady Wirjanata; Boni F Sebayang; Ric N Price; Arnab Chatterjee; Advait Nagle; Marcin Stasiak; Susan A Charman; Iñigo Angulo-Barturen; Santiago Ferrer; María Belén Jiménez-Díaz; María Santos Martínez; Francisco Javier Gamo; Vicky M Avery; Andrea Ruecker; Michael Delves; Kiaran Kirk; Matthew Berriman; Sandhya Kortagere; Jeremy Burrows; Erkang Fan; Lawrence W Bergman

doi:10.1038/ncomms6521

Pyrazoleamide compounds are potent antimalarials that target Na+ homeostasis in intraerythrocytic Plasmodium falciparum

Nat Commun. 2014 Nov 25:5:5521. doi: 10.1038/ncomms6521.

Authors

Akhil B Vaidya¹, Joanne M Morrisey¹, Zhongsheng Zhang², Sudipta Das¹, Thomas M Daly¹, Thomas D Otto³, Natalie J Spillman⁴, Matthew Wyvratt⁵, Peter Siegl⁵, Jutta Marfurt⁶, Grennady Wirjanata⁶, Boni F Sebayang⁷, Ric N Price⁸, Arnab Chatterjee⁹, Advait Nagle⁹, Marcin Stasiak², Susan A Charman¹⁰, Iñigo Angulo-Barturen¹¹, Santiago Ferrer¹¹, María Belén Jiménez-Díaz¹¹, María Santos Martínez¹¹, Francisco Javier Gamo¹¹, Vicky M Avery¹², Andrea Ruecker¹³, Michael Delves¹³, Kiaran Kirk⁴, Matthew Berriman³, Sandhya Kortagere¹, Jeremy Burrows⁵, Erkang Fan², Lawrence W Bergman¹

Affiliations

¹ Department of Microbiology and Immunology, Center for Molecular Parasitology, Drexel University College of Medicine, 2900 Queen Lane, Philadelphia, Pennsylvania 190129, USA.
² Department of Biochemistry, University of Washington, Box 357350, Seattle, Washington 98195, USA.
³ Wellcome Trust Sanger Institute, Hinxton, Cambridge CB101SA, UK.
⁴ Research School of Biology, The Australian National University, Canberra, Australian Capital Territory 0200, Australia.
⁵ Medicines for Malaria Venture, PO Box 1826, 20Rt de Pr-Bois, Geneva 15 1215, Switzerland.
⁶ Division of Global and Tropical Health, Menzies School of Health Research and Charles Darwin University, PO Box 41096, Casuarina, Northern Territory 0811, Australia.
⁷ Eijkman Institute for Molecular Biology, Jl. Diponegoro 69, Jakarta 10430, Indonesia.
⁸ 1] Division of Global and Tropical Health, Menzies School of Health Research and Charles Darwin University, PO Box 41096, Casuarina, Northern Territory 0811, Australia [2] Nuffield Department of Clinical Medicine, Centre for Tropical Medicine, University of Oxford, Oxford OX3 7LJ, UK.
⁹ Genomics Institute of the Novartis Research Foundation, 10675 John Jay Hopkins Drive, San Diego, California 92121, USA.
¹⁰ Center for Drug Candidate Optimisation, Monash University, 381 Royal Parade, Parkville, Victoria 3052, Australia.
¹¹ GlaxoSmithKline, Malaria Support Group, Calle Severo Ochoa 2, Tres Cantos 28760, Spain.
¹² Eskitis Institute, Griffith University, Don Young Road, Nathan, Queensland 4111, Australia.
¹³ Department of Life Sciences, South Kensington Campus, Imperial College, London SW7 2AZ, UK.

Abstract

The quest for new antimalarial drugs, especially those with novel modes of action, is essential in the face of emerging drug-resistant parasites. Here we describe a new chemical class of molecules, pyrazoleamides, with potent activity against human malaria parasites and showing remarkably rapid parasite clearance in an in vivo model. Investigations involving pyrazoleamide-resistant parasites, whole-genome sequencing and gene transfers reveal that mutations in two proteins, a calcium-dependent protein kinase (PfCDPK5) and a P-type cation-ATPase (PfATP4), are necessary to impart full resistance to these compounds. A pyrazoleamide compound causes a rapid disruption of Na(+) regulation in blood-stage Plasmodium falciparum parasites. Similar effect on Na(+) homeostasis was recently reported for spiroindolones, which are antimalarials of a chemical class quite distinct from pyrazoleamides. Our results reveal that disruption of Na(+) homeostasis in malaria parasites is a promising mode of antimalarial action mediated by at least two distinct chemical classes.

Publication types

Research Support, N.I.H., Extramural
Research Support, Non-U.S. Gov't

MeSH terms

Adenosine Triphosphatases / genetics
Adenosine Triphosphatases / metabolism
Amides / pharmacology*
Antimalarials / pharmacology*
Benzimidazoles / pharmacology*
Erythrocytes / parasitology*
Female
Homeostasis / drug effects
Humans
Malaria / parasitology*
Male
Plasmodium berghei / drug effects
Plasmodium berghei / genetics
Plasmodium berghei / metabolism
Plasmodium falciparum / drug effects*
Plasmodium falciparum / enzymology
Plasmodium falciparum / genetics
Plasmodium falciparum / metabolism
Protein Kinases / genetics
Protein Kinases / metabolism
Protozoan Proteins
Pyrazoles / pharmacology*
Sodium / metabolism*

Substances

Amides
Antimalarials
Benzimidazoles
PA21A050
Protozoan Proteins
Pyrazoles
pyrazole
Sodium
Protein Kinases
calcium-dependent protein kinase
Adenosine Triphosphatases

Associated data

PubChem-Substance/221675649
PubChem-Substance/221675650
PubChem-Substance/221675651

Abstract

Publication types

MeSH terms

Substances

Associated data

Grants and funding