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Characterization of the ATP4 ion pump in Toxoplasma gondii

Authors :
Lehane, AM
Dennis, ASM
Bray, KO
Li, D
Rajendran, E
McCoy, JM
McArthur, HM
Winterberg, M
Rahimi, F
Tonkin, CJ
Kirk, K
van Dooren, GG
Lehane, AM
Dennis, ASM
Bray, KO
Li, D
Rajendran, E
McCoy, JM
McArthur, HM
Winterberg, M
Rahimi, F
Tonkin, CJ
Kirk, K
van Dooren, GG
Publication Year :
2019

Abstract

The Plasmodium falciparum ATPase PfATP4 is the target of a diverse range of antimalarial compounds, including the clinical drug candidate cipargamin. PfATP4 was originally annotated as a Ca2+ transporter, but recent evidence suggests that it is a Na+ efflux pump, extruding Na+ in exchange for H+ Here we demonstrate that ATP4 proteins belong to a clade of P-type ATPases that are restricted to apicomplexans and their closest relatives. We employed a variety of genetic and physiological approaches to investigate the ATP4 protein of the apicomplexan Toxoplasma gondii, TgATP4. We show that TgATP4 is a plasma membrane protein. Knockdown of TgATP4 had no effect on resting pH or Ca2+ but rendered parasites unable to regulate their cytosolic Na+ concentration ([Na+]cyt). PfATP4 inhibitors caused an increase in [Na+]cyt and a cytosolic alkalinization in WT but not TgATP4 knockdown parasites. Parasites in which TgATP4 was knocked down or disrupted exhibited a growth defect, attributable to reduced viability of extracellular parasites. Parasites in which TgATP4 had been disrupted showed reduced virulence in mice. These results provide evidence for ATP4 proteins playing a key conserved role in Na+ regulation in apicomplexan parasites.

Details

Database :
OAIster
Publication Type :
Electronic Resource
Accession number :
edsoai.on1397540896
Document Type :
Electronic Resource