Dematin,a human erythrocyte cytoskeletal protein,is a substrate for a recombinant FIKK kinase from Plasmodium falciparum |
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| Authors: | Gabriel S. Brandt Scott Bailey |
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| Affiliation: | Department of Biochemistry and Molecular Biology, Johns Hopkins University, Bloomberg School of Public Health, Baltimore, MD 21205, United States |
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| Abstract: | P. falciparum causes the most deadly form of malaria, resulting from the adherence of infected red blood cells to blood vessels. During the blood stage of infection, the parasite secretes a large number of proteins into the host erythrocyte. The secretion of a 20-member family of protein kinases known as FIKK kinases, after a conserved Phe-Ile-Lys-Lys sequence motif, is unique to P. falciparum. Identification of physiological substrates of these kinases may provide perspective on the importance of FIKK kinase activity to P. falciparum virulence. We demonstrate, for the first time, the heterologous expression and purification of a FIKK kinase (PfFk4.1, PFD1165w). The recombinant kinase is active against general substrates and phosphorylates itself. Having demonstrated kinase activity, we incubated recombinant Fk4.1 with parasite and human erythrocyte lysates. No parasite-derived substrates were identified. However, treatment of erythrocyte ghosts shows that the FIKK kinase Fk4.1 phosphorylates dematin, a cytoskeletal protein found at the red blood cell spectrin–actin junction. |
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| Keywords: | FIKK kinase, Phe-Ile-Lys-Lys-containing kinase Pf, Plasmodium falciparum PfFk, FIKK kinase from P. falciparum PEXEL, plasmodium export element Fk8, FIKK kinase encoded on chromosome 8 Fk4.1k, kinase domain of Fk4.1 KESTREL, kinase substrate tracking and elucidation IMAC, immobilized metal affinity chromatography JHMRI, Johns Hopkins Bloomberg School of Public Health Malaria Research Institute iRBC, infected red blood cell PDB, Protein Data Bank GLUT1, glucose transporter 1 WHO, World Health Organization |
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