Abstract
BackgroundThe widespread protozoan parasite Toxoplasma gondii interferes with host cell functions by exporting the contents of a unique apical organelle, the rhoptry. Among the mix of secreted proteins are an expanded, lineage-specific family of protein kinases termed rhoptry kinases (ROPKs), several of which have been shown to be key virulence factors, including the pseudokinase ROP5. The extent and details of the diversification of this protein family are poorly understood.ResultsIn this study, we comprehensively catalogued the ROPK family in the genomes of Toxoplasma gondii, Neospora caninum and Eimeria tenella, as well as portions of the unfinished genome of Sarcocystis neurona, and classified the identified genes into 42 distinct subfamilies. We systematically compared the rhoptry kinase protein sequences and structures to each other and to the broader superfamily of eukaryotic protein kinases to study the patterns of diversification and neofunctionalization in the ROPK family and its subfamilies. We identified three ROPK sub-clades of particular interest: those bearing a structurally conserved N-terminal extension to the kinase domain (NTE), an E. tenella-specific expansion, and a basal cluster including ROP35 and BPK1 that we term ROPKL. Structural analysis in light of the solved structures ROP2, ROP5, ROP8 and in comparison to typical eukaryotic protein kinases revealed ROPK-specific conservation patterns in two key regions of the kinase domain, surrounding a ROPK-conserved insert in the kinase hinge region and a disulfide bridge in the kinase substrate-binding lobe. We also examined conservation patterns specific to the NTE-bearing clade. We discuss the possible functional consequences of each.ConclusionsOur work sheds light on several important but previously unrecognized features shared among rhoptry kinases, as well as the essential differences between active and degenerate protein kinases. We identify the most distinctive ROPK-specific features conserved across both active kinases and pseudokinases, and discuss these in terms of sequence motifs, evolutionary context, structural impact and potential functional relevance.By characterizing the proteins that enable these parasites to invade the host cell and co-opt its signaling mechanisms, we provide guidance on potential therapeutic targets for the diseases caused by coccidian parasites.
Highlights
The widespread protozoan parasite Toxoplasma gondii interferes with host cell functions by exporting the contents of a unique apical organelle, the rhoptry
We mapped the sites and regions of interest onto solved structures of ROP2, ROP8 and ROP5 to examine the structural and possible functional roles these features may play within the parasite proteins
Global trends in the rhoptry kinases (ROPKs) family We used a set of HMM profiles derived from our subfamily sequence alignments to scan the translated gene model sequences available for T. gondii strains GT1, ME49 and VEG, N. caninum and E. tenella and classify putative ROPK genes into the identified subfamilies
Summary
The widespread protozoan parasite Toxoplasma gondii interferes with host cell functions by exporting the contents of a unique apical organelle, the rhoptry. Toxoplasma gondii is an intracellular parasite that infects a wide range of hosts, including an estimated one-third of the world’s human population [1]. T. gondii and its evolutionary relatives, the Coccidia, form a clade of parasitic protozoa involved in many human and veterinary diseases such as toxoplasmosis and coccidiosis. At the initiation of host cell invasion, the contents of the rhoptries are injected into the host cell and the forming parasitophorous vacuole which protects the intracellular parasite [6]. The parasite proteins can disrupt host cell signaling and defense mechanisms and assist in recruiting host organelles [7]
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