PfAP2-MRP DNA-binding protein is a master regulator of parasite pathogenesis during malaria parasite blood stages

  1. Amit Kumar Subudhi
  2. Judith L. Green
  3. Rohit Satyam
  4. Todd Lenz
  5. Rahul P. Salunke
  6. Muhammad Shuaib
  7. Ioannis Isaioglou
  8. Steven Abel
  9. Mohit Gupta
  10. Luke Esau
  11. Tobias Mourier
  12. Raushan Nugmanova
  13. Sara Mfarrej
  14. Rupali Sivapurkar
  15. Zenaida Stead
  16. Fathia Ben Rached
  17. Yogesh Otswal
  18. Rachid Sougrat
  19. Ashraf Dada
  20. Abdullah Fuaad Kadamany
  21. Wolfgang Fischle
  22. Jasmeen Merzaban
  23. Ellen Knuepfer
  24. David J.P. Ferguson
  25. Ishaan Gupta
  26. Karine G. Le Roch
  27. Anthony A. Holder
  28. Arnab Pain
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Abstract

Malaria pathogenicity results from the parasite’s ability to invade, multiply within and then egress from the host red blood cell (RBC). Infected RBCs are remodeled, expressing antigenic variant proteins (such as PfEMP1, coded by the var gene family) for immune evasion and survival. These processes require the concerted actions of many proteins, but the molecular regulation is poorly understood. We have characterized an essential Plasmodium specific Apicomplexan AP2 (ApiAP2) transcription factor in Plasmodium falciparum (PfAP2-MRP; Master Regulator of Pathogenesis) during the intraerythrocytic developmental cycle (IDC). An inducible gene knockout approach showed that PfAP2-MRP is essential for development during the trophozoite stage, and critical for var gene regulation, merozoite development and parasite egress. ChIP-seq experiments performed at 16 hour post invasion (h.p.i.) and 40 h.p.i. matching the two peaks of PfAP2-MRP expression, demonstrate binding of PfAP2-MRP to the promoters of genes controlling trophozoite development and host cell remodeling at 16 h.p.i. and antigenic variation and pathogenicity at 40 h.p.i. Using single-cell RNA-seq and fluorescence-activated cell sorting, we show de-repression of most var genes in Δpfap2-mrp parasites that express multiple PfEMP1 proteins on the surface of infected RBCs. In addition, the Δpfap2-mrp parasites overexpress several early gametocyte marker genes at both 16 and 40 h.p.i., indicating a regulatory role in the sexual stage conversion. Using the Chromosomes Conformation Capture experiment (Hi-C), we demonstrate that deletion of PfAP2-MRP results in significant reduction of both intra-chromosomal and inter-chromosomal interactions in heterochromatin clusters. We conclude that PfAP2-MRP is a vital upstream transcriptional regulator controlling essential processes in two distinct developmental stages during the IDC that include parasite growth, chromatin structure and var gene expression.

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  1. Version published to 10.1101/2023.05.23.541898v1 on bioRxiv