Inhibitors of ApiAP2 protein DNA binding exhibit multistage activity against Plasmodium parasites

Author:

Russell Timothy JamesORCID,De Silva Erandi K.,Crowley Valerie M.,Shaw-Saliba Kathryn,Dube Namita,Josling Gabrielle,Pasaje Charisse Flerida A.,Kouskoumvekaki Irene,Panagiotou Gianni,Niles Jacquin C.,Jacobs-Lorena Marcelo,Denise Okafor C.,Gamo Francisco-Javier,Llinás ManuelORCID

Abstract

Plasmodium parasites are reliant on the Apicomplexan AP2 (ApiAP2) transcription factor family to regulate gene expression programs. AP2 DNA binding domains have no homologs in the human or mosquito host genomes, making them potential antimalarial drug targets. Using an in-silico screen to dock thousands of small molecules into the crystal structure of the AP2-EXP (Pf3D7_1466400) AP2 domain (PDB:3IGM), we identified putative AP2-EXP interacting compounds. Four compounds were found to block DNA binding by AP2-EXP and at least one additional ApiAP2 protein. Our top ApiAP2 competitor compound perturbs the transcriptome of P. falciparum trophozoites and results in a decrease in abundance of log2 fold change > 2 for 50% (46/93) of AP2-EXP target genes. Additionally, two ApiAP2 competitor compounds have multi-stage anti-Plasmodium activity against blood and mosquito stage parasites. In summary, we describe a novel set of antimalarial compounds that interact with AP2 DNA binding domains. These compounds may be used for future chemical genetic interrogation of ApiAP2 proteins or serve as starting points for a new class of antimalarial therapeutics.

Funder

Division of Intramural Research, National Institute of Allergy and Infectious Diseases

Center for Quantitative Biology

NIH

Sir Keith Murdoch Fellowship

American Heart Association

Publisher

Public Library of Science (PLoS)

Subject

Virology,Genetics,Molecular Biology,Immunology,Microbiology,Parasitology

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