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CDC50 Orthologues in Plasmodium falciparum Have Distinct Roles in Merozoite Egress and Trophozoite Maturation

Avnish Patel, Stephanie D. Nofal, Michael J. Blackman, David A. Baker

2022mBio19 citationsDOIOpen Access PDF

Abstract

parasites within red blood cells. Mature daughter merozoites are released from infected erythrocytes to invade new cells in a tightly regulated process termed egress. Previous studies have shown that a unique bifunctional guanylyl cyclase, GCα, initiates egress by synthesis of cGMP. GCα has an N-terminal P4-ATPase domain of unknown function. In model organisms, P4-ATPases function through interaction with a CDC50 partner protein. Here, we investigate the role of CDC50 orthologues in P. falciparum and show that GCα binds CDC50B, an interaction that regulates egress efficiency. We also find that CDC50C is essential and binds a putative P4-ATPase, ATP2, in a complex that influences endocytosis of host hemaglobin. Our results highlight the heterogenous and critical role of CDC50 proteins in P. falciparum.

Topics & Concepts

Plasmodium falciparumBiologyCell biologyATPasePlasmodium (life cycle)BiochemistryParasite hostingMalariaEnzymeImmunologyComputer scienceWorld Wide WebMalaria Research and ControlParasites and Host InteractionsTrypanosoma species research and implications