Endogenous structure of antimalarial target Pf ATP4 reveals new class of apicomplexan P-type ATPase modulators

Meseret T. Haile
Anurag Shukla
James Zhen
Michael W. Mather
Suyash Bhatnagar
Zhening Zhang
Akhil B. Vaidya
Chi-Min Ho

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Abstract

The Plasmodium falciparum sodium efflux pump Pf ATP4 is a leading antimalarial target, but suffers from a lack of high-resolution structural information needed to identify functionally important features in conserved regions and guide rational design of next generation inhibitors. Here, we determine a 3.7Å cryoEM structure of Pf ATP4 purified from CRISPR-engineered P. falciparum parasites, revealing a previously unknown, apicomplexan-specific binding partner, Pf ABP, which forms a conserved, likely modulatory interaction with Pf ATP4. The discovery of Pf ABP presents a new avenue for designing novel Pf ATP4 inhibitors.

Version published to 10.1101/2025.02.25.640208v1 on bioRxiv
Feb 25, 2025

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Aryl N-acetamide compounds exert antimalarial activity by acting as agonists of rhomboid protease Pf ROM8 and cation channel Pf CSC1

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