A forward genetic approach to identifying novel calcium regulators in Toxoplasma Gondii

LaFavers, Kaice Arminda

25 July 2017

Indiana University-Purdue University Indianapolis (IUPUI) / Toxoplasma gondii is an obligate intracellular eukaryotic pathogen that causes severe neurologic disease in immunocompromised adults and congenitally infected neonates. Events critical to the propagation of T. gondii, such as invasion and egress, are regulated by calcium-dependent signaling. In order to identify unique components of the parasite’s calcium signaling networks, members of the Arrizabalaga laboratory have used a forward genetics approach to isolate mutants with altered sensitivity to the calcium ionophore A23187. Exposing extracellular parasites to A23187 induces protein secretion, motility and cytoskeletal rearrangements and prolonged treatment causes exhaustion of factors required for invasion, which results in what is referred to as ionophore induced death (iiDeath). Mutants capable of surviving this treatment were isolated from a chemically mutagenized population. Whole genome sequencing of one such mutant, MBD2.1, identified a nonsense mutation in a protein of unknown function (TGGT1_069070, ToxoDBv7.2) Complementation of MBD 2.1 with a wild-type copy of TGGT1_069070 restored sensitivity to iiDeath treatment. Endogenous tagging of this locus revealed that the encoded protein is secreted from a unique parasite secretory organelle known as the dense granule into the parasitophorous vacuole, leading to its designation as TgGRA41. Complete knockout of TgGRA41 recapitulates the resistance to iiDeath observed in MBD2.1 but also exhibits a dramatic decrease in propagation in tissue culture not seen in the original mutant. The knockout shows defects in multiple steps of the lytic including compromised invasion efficiency and premature egress of parasites from host cells. Cytosolic calcium measurements of extracellular parasites show enhanced uptake of calcium in the knockout strain as compared to parental and complemented, suggesting that the loss of TgGra41 results in calcium dysregulation. Together, these results provide a novel insight into the role that the parasitophorous vacuole of T. gondii plays in calcium homeostasis and calcium-dependent signaling processes.

Toxoplasma gondii

Calcium

Dense granule

Parasite

Platelets and Serotonin in Migraine

Chang, Karin

05 August 2010

No description available.

Biomedical Research

Neurology

platelet

serotonin

migraine

headache

bleeding

dense granule

Molecular Mechanisms Underlying Differential Regulation of Platelet Dense Granule Secretion by Protein Kinase C delta

Chari, Ramya

January 2010

Protein Kinase C delta (PKCδ) is expressed in platelets and activated downstream of protease-activated receptors (PAR)s and glycoprotein VI (GPVI) receptors. We evaluated the role of PKCδ in platelets using two approaches - pharmacological and molecular genetic approach. In human platelets pretreated with isoform selective antagonistic RACK peptide (δV1-1)TAT, and in the murine platelets lacking PKCδ, PAR4-mediated dense granule secretion was inhibited, whereas GPVI-mediated dense granule secretion was potentiated. These effects were statistically significant in the absence and presence of thromboxane A2 (TXA2). Furthermore, TXA2 generation was differentially regulated by PKCδ. However, PKCδ had a small effect on platelet P-selectin expression. Calcium- and PKC-dependent pathways independently activate fibrinogen receptor in platelets. When calcium pathways are blocked by dimethyl-BAPTA, AYPGKF-induced aggregation in PKCδ null mouse platelets and in human platelets pretreated with (δV1-1)TAT, was inhibited. In a FeCl3-induced injury in vivo thrombosis model, PKCδ-/- mice occluded similar to their wild-type littermates. Hence, we conclude that PKCδ differentially regulates platelet functional responses such as dense granule secretion and TXA2 generation downstream of PARs and GPVI receptors, but PKCδ deficiency does not affect the thrombus formation in vivo. We further investigated the mechanism of such differential regulation of dense granule release by PKCδ in platelets. SH2 domain-containing Inositol Phosphatase (SHIP)-1 is phosphorylated on Y1020, a marker for its activation, upon stimulation of human platelets with PAR agonists, SFLLRN and AYPGKF, or GPVI agonist, convulxin. GPVImediated SHIP-1 phosphorylation occurred rapidly at 15 sec whereas PAR-mediated phosphorylation was delayed, occurring at 1 min. Lyn and SHIP-1, but not SHIP-2 or Shc, preferentially associated with PKCδ upon stimulation of platelets with a GPVI agonists, but not with a PAR agonist. In PKCδ null murine platelets, convulxin-induced SHIP-1 phosphorylation was inhibited, suggesting that PKCδ regulates the phosphorylation of SHIP-1. Furthermore, in Lyn null murine platelets, GPVI-mediated phosphorylations on Y-1020 of SHIP-1, Y311 and Y155 of PKCδ were inhibited. In murine platelets lacking Lyn, or SHIP-1, GPVI-mediated dense granule secretions were potentiated, whereas PAR-mediated dense granule secretions were inhibited. Phosphorylated SHIP-1 associated with phosphorylated-Y155 PKCδ peptide. Therefore, we conclude that Lyn-mediated phosphorylations of PKCδ and SHIP-1 and their associations negatively regulate GPVI-mediated dense granule secretion in platelets. / Physiology

Biology, Physiology

Biology, Cell

Biology, Molecular

Dense Granule Secretion

Phosphorylation

Platelets

Protein Kinase C

Signaling

Thrombosis

Diagnostic des pathologies plaquettaires : optimisation de l'exploration des granules denses plaquettaires / Diagnosis of platelet disorders : improvement in the assessment of platelet dense granules

Cai, Huili

06 July 2015

Les plaquettes sont les cellules principales de l’hémostase. Leur anomalie qualitative et/ou quantitative est à l’origine d’une diathèse hémorragique. Le diagnostic des anomalies plaquettaires nécessite des tests biologiques. L’objectif de notre travail a été d’améliorer leur diagnostic, en particulier, de développer de nouveaux outils d’exploration des granules denses plaquettaires. Les pathologies plaquettaires héréditaires sont mal connues en Chine. Donc la cadre de notre collaboration Nancy /Wuhan nous avons publié un article en Chinois sur les thrombopénies héréditaires. Ensuite, nous avons évalué les performances du test à la mépacrine combiné à l’expression de CD63 par cytométrie en flux (CMF) pour le diagnostic de la pathologie des grains denses plaquettaires. De plus, notre étude montre que la carence de vitamine C pourrait être associée à une thrombopathie des grains denses. Enfin, nous avons développé une approche par CMF, puis par HPLC, pour la détection de sérotonine plaquettaire / Platelets play an essential role in the hemostasis. Abnormalities in platelet number or platelet function may result in excessive bleeding. Diagnosis of platelet disorders requires platelet count and platelet function testing. Our work is aimed to improve the diagnosis of platelet disorders, especially to develop new approaches for testing the function of platelet dense granules. Inherited platelet disorders are hardly recognized in China. Therefore we published an article in Chinese on the topic of hereditary thrombocytopenia in a Chinese clinical journal, within the framework of collaboration between Nancy and Wuhan. In addition, we evaluated the usefulness of flow cytometric mepacrine assay combined with CD63 expression in the diagnosis of dense granule disorder. Moreover, our work demonstrates that vitamin C deficiency might be associated with platelet dense granule disorder. Finally, we developed a method by flow cytometry and then by HPLC for detection of platelet serotonin

Pathologies plaquettaires

Pathologie des grains denses

Maladie de pool vide delta

Vitamine C

Sérotonine plaquettaire

Cytométrie en flux

Platelet disorders

Dense granule disorder

Vitamin C

Platelet serotonin

Flow cytometry

612.117

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