Tatsuya Iwanaga scite author profile

BackgroundcAMP-dependent protein kinase (PKA) has been implicated in the asexual stage of the Toxoplasma gondii life cycle through assaying the effect of a PKA-specific inhibitor on its growth rate. Since inhibition of the host cell PKA cannot be ruled out, a more precise evaluation of the role of PKA, as well as characterization of the kinase itself, is necessary.Methodology/Principal FindingThe inhibitory effects of two PKA inhibitors, H89, an ATP-competitive chemical inhibitor, and PKI, a substrate-competitive mammalian natural peptide inhibitor, were estimated. In the in vitro kinase assay, the inhibitory effect of PKI on a recombinant T. gondii PKA catalytic subunit (TgPKA-C) was weaker compared to that on mammalian PKA-C. In a tachyzoite growth assay, PKI had little effect on the growth of tachyzoites, whereas H89 strongly inhibited it. Moreover, T. gondii PKA regulatory subunit (TgPKA-R)-overexpressing tachyzoites showed a significant growth defect.Conclusions/SignificanceOur data suggest that PKA plays an important role in the growth of tachyzoites, and the inhibitory effect of substrate-competitive inhibitor PKI on T. gondii PKA was low compared to that of the ATP competitive inhibitor H89.

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Analyses of Interactions Between Heparin and the Apical Surface Proteins of Plasmodium falciparum

Kobayashi

Takano

Takemae

et al. 2013

Sci Rep

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Heparin, a sulfated glycoconjugate, reportedly inhibits the blood-stage growth of the malaria parasite Plasmodium falciparum. Elucidation of the inhibitory mechanism is valuable for developing novel invasion-blocking treatments based on heparin. Merozoite surface protein 1 has been reported as a candidate target of heparin; however, to better understand the molecular mechanisms involved, we characterized the molecules that bind to heparin during merozoite invasion. Here, we show that heparin binds only at the apical tip of the merozoite surface and that multiple heparin-binding proteins localize preferentially in the apical organelles. To identify heparin-binding proteins, parasite proteins were fractionated by means of heparin affinity chromatography and subjected to immunoblot analysis with ligand-specific antibodies. All tested members of the Duffy and reticulocyte binding-like families bound to heparin with diverse affinities. These findings suggest that heparin masks the apical surface of merozoites and blocks interaction with the erythrocyte membrane after initial attachment.

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Superoxide scavenging activity of pirfenidone–iron complex

Mitani

Sato

Muramoto

et al. 2008

Biochemical and Biophysical Research Communications

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Identification of mutations in TgMAPK1 of Toxoplasma gondii conferring resistance to 1NM-PP1

Sugi

Kobayashi

Takemae

et al. 2013

International Journal for Parasitology: Drugs and Drug Resistan

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Tatsuya Iwanaga

Identification of Toxoplasma gondii cAMP Dependent Protein Kinase and Its Role in the Tachyzoite Growth

Analyses of Interactions Between Heparin and the Apical Surface Proteins of Plasmodium falciparum

Superoxide scavenging activity of pirfenidone–iron complex

Identification of mutations in TgMAPK1 of Toxoplasma gondii conferring resistance to 1NM-PP1

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