Literature DB >> 26859096

The FIKK kinase of Toxoplasma gondii is not essential for the parasite's lytic cycle.

S Skariah1, O Walwyn2, K Engelberg3, M-J Gubbels3, C Gaylets2, N Kim2, B Lynch2, A Sultan1, D G Mordue4.   

Abstract

FIKK kinases are a novel family of kinases unique to the Apicomplexa. While most apicomplexans encode a single FIKK kinase, Plasmodium falciparum expresses 21 and piroplasms do not encode a FIKK kinase. FIKK kinases share a conserved C-terminal catalytic domain, but the N-terminal region is highly variable and contains no known functional domains. To date, FIKK kinases have been primarily studied in P. falciparum and Plasmodium berghei. Those that have been studied are exported from the parasite and associate with diverse locations in the infected erythrocyte cytosol or membrane. Deletion of individual P. falciparum FIKK kinases indicates that they may play a role in modification of the infected erythrocyte. The current study characterises the single FIKK gene in Toxoplasma gondii to evaluate the importance of the FIKK kinase in an apicomplexan that has a single FIKK kinase. The TgFIKK gene encoded a protein of approximately 280kDa. Endogenous tagging of the FIKK protein with Yellow Fluorescent Protein showed that the FIKK protein exclusively localised to the posterior end of tachyzoites. A Yellow Fluorescent Protein-tagged FIKK and a Ty-tagged FIKK both co-localised with T. gondii membrane occupation and recognition nexus protein to the basal complex and were localised apical to inner membrane complex protein-5 and Centrin2. Deletion of TgFIKK, surprisingly, had no detectable effect on the parasite's lytic cycle in vitro in human fibroblast cells or in acute virulence in vivo. Thus, our results clearly show that while the FIKK kinase is expressed in tachyzoites, it is not essential for the lytic cycle of T. gondii.
Copyright © 2016 Australian Society for Parasitology Inc. Published by Elsevier Ltd. All rights reserved.

Entities:  

Keywords:  Basal complex; FIKK kinase; Intracellular pathogen; Parasite; Serine threonine kinases; Toxoplasma

Mesh:

Substances:

Year:  2016        PMID: 26859096      PMCID: PMC4844859          DOI: 10.1016/j.ijpara.2016.01.001

Source DB:  PubMed          Journal:  Int J Parasitol        ISSN: 0020-7519            Impact factor:   3.981


  26 in total

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2.  FIKK Kinase, a Ser/Thr Kinase Important to Malaria Parasites, Is Inhibited by Tyrosine Kinase Inhibitors.

Authors:  Benjamin C Lin; Darcy R Harris; Lucy M D Kirkman; Astrid M Perez; Yiwen Qian; Janse T Schermerhorn; Min Y Hong; Dennis S Winston; Lingyin Xu; Gabriel S Brandt
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