Prostacyclin inhibits platelet aggregation induced by phorbol ester or Ca2+ ionophore at steps distal to activation of protein kinase C and Ca2+-dependent protein kinases

Siess, Wolfgang; Lapetina, Eduardo G.

doi:10.1042/bj2580057

Cited by 44 publications

(20 citation statements)

References 52 publications

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“…The observation that phosphorylation of p47 is increased in thrombin-and PAF-treated platelets has been used to argue that agonist-induced PIP2 turnover is coupled to PKC activation (Ieyasu et al, 1982;Sano et al, 1983). However, PGI2 and cAMP-analogue treatments of platelets block PAF-, thrombin-and fluoride-induced p47 phosphorylation (Ieyasu , 1982;Sano et al, 1983;Kroll et al, 1988;Siess & Lapetina, 1989;Lazarowski & Lapetina, 1989), even though PIP2 breakdown in response to thrombin was not sensitive to up to 50 ,ug of PGI2/ml (Fig. 4).…”

Section: Discussionmentioning

confidence: 99%

“…267 Indeed, recent studies with human platelets (Doni et al, 1988;Kroll et al, 1988;Siess & Lapetina, 1989) …”

Section: Discussionmentioning

confidence: 99%

“…Phosphorylation-induced retardation of proteins on SDS/PAGE gels has been described previously (Casnellie, 1987). PGI2 treatment leads to the appearance of a 50 kDa phosphoprotein on SDS/PAGE gels of platelet extracts (Siess & Lapetina, 1989). Analysis of the amino acid sequence of the p47 protein reveals the presence of at least five classic consensus sequences for PKA phosphorylation (i.e.…”

Section: Discussionmentioning

confidence: 99%

“…Via activation of adenylate cyclase, it elevates the level of cyclic AMP (cAMP) in platelets, and this leads to a stimulation of cAMP-dependent protein kinase (PKA) activity. At least two sites of PKA action in the disruption of agonistinduced platelet aggregation have been distinguished, and these are pre-and post-PKC activation (Kroll et al, 1988;Siess & Lapetina, 1989). PGI2 and cAMP-analogue treatment of platelets leads to an inhibition of agonist-stimulated PIP2 breakdown, perhaps via PKA phosphorylation of a putative GTP-binding protein (G-protein) which couples the agonist receptors to phospholipase C (Halenda & Feinstein, 1984;Ieyasu et al, 1982;Doni et al, 1988;Lazarowski & Lapetina, 1989;Yada et al, 1989).…”

Section: Introductionmentioning

confidence: 99%

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Translocation-independent activation of protein kinase C by platelet-activating factor, thrombin and prostacyclin. Lack of correlation with polyphosphoinositide hydrolysis in rabbit platelets

Salari

Duronio

Howard

et al. 1990

Biochemical Journal

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The relationship between polyphosphoinositide hydrolysis and protein kinase C (PKC) activation was explored in rabbit platelets treated with the agonists platelet-activating factor (PAF), thrombin and 12-O-tetradecanoylphorbol 13-acetate (TPA), and with the anti-aggregant prostacyclin (PGI2). Measurement of the hydrolysis of radiolabelled inositolcontaining phospholipids relied upon the separation of the products [3H]inositol mono-, bis-and tris-phosphates by Dowex-l chromatography. PKC activity, measured in platelet cytosolic and Nonidet-P40-solubilized particulate extracts that were fractionated by MonoQ chromatography, was based upon the ability of the enzyme to phosphorylate either histone HI in the presence of the activators Ca2+, diacylglycerol and phosphatidylserine, or protamine in the absence of Ca2+ and lipid. Treatment of platelets for 1 min with PAF (2 nM) or thrombin (2 units/ml) led to the rapid hydrolysis of inositol-containing phospholipids, a 2-3-fold stimulation of both cytosolic and particulate-derived PKC activity, and platelet aggregation. Exposure to TPA (200 nM) for 5 min did not stimulate formation of phosphoinositides, but translocated more than 95 % of cytosolic PKC into the particulate fraction, and induced a slower rate of aggregation. PGI2 (1 ,ug/ml) did not enhance phosphoinositide production, and at higher concentrations (50 ,ug/ml) it antagonized the ability of PAF, but not that of thrombin, to induce inositol phospholipid turnover, even though platelet aggregation in response to both agonists was blocked by PGI2. On the other hand, PGI2 alone also appeared to activate (by 3-5-fold) cytosolic and particulate PKC by a translocation-independent mechanism. The activation of PKC by PGI2 was probably mediated via cyclic AMP (cAMP), as this effect was mimicked by the cAMP analogue 8-chlorophenylthio-cAMP. It is concluded that this novel mechanism of PKC regulation by platelet agonists may operate independently of polyphosphoinositide turnover, and that activation of cAMP-dependent protein kinase represents another route leading to PKC activation.

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Section: Discussionmentioning

confidence: 99%

“…267 Indeed, recent studies with human platelets (Doni et al, 1988;Kroll et al, 1988;Siess & Lapetina, 1989) …”

Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 2 more Smart Citations

Translocation-independent activation of protein kinase C by platelet-activating factor, thrombin and prostacyclin. Lack of correlation with polyphosphoinositide hydrolysis in rabbit platelets

Salari

Duronio

Howard

et al. 1990

Biochemical Journal

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“…In the presence of cAMP, the activation of phospholipase C (and hence the production of InsP 3 and diacylglycerol) by the agonist is depressed, leading to the inhibition of the increment of [Ca 2ϩ ] i and of PKC-dependent phosphorylations (21). The action of cAMP is also on events distal to the activation of phospholipase C since platelet aggregation and secretion induced by the Ca 2ϩ ionophore ionomycin or by phorbol esters are also inhibited by the cyclic nucleotide (22)(23)(24). cAMP also increases the incorporation of diacylglycerol into phosphatidylinositol (25).…”

mentioning

confidence: 99%

Prostacyclin and Sodium Nitroprusside Inhibit the Activity of the Platelet Inositol 1,4,5-Trisphosphate Receptor and Promote Its Phosphorylation

Cavallini

Coassin

Borean

et al. 1996

Journal of Biological Chemistry

131

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Platelet‐Activation Mechanisms and Vascular Remodeling

Rubenstein

Yin

2018

Comprehensive Physiology

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This overview article for the Comprehensive Physiology collection is focused on detailing platelets, how platelets respond to various stimuli, how platelets interact with their external biochemical environment, and the role of platelets in physiological and pathological processes. Specifically, we will discuss the four major functions of platelets: activation, adhesion, aggregation, and inflammation. We will extend this discussion to include various mechanisms that can induce these functional changes and a discussion of some of the salient receptors that are responsible for platelets interacting with their external environment. We will finish with a discussion of how platelets interact with their vascular environment, with a special focus on interactions with the extracellular matrix and endothelial cells, and finally how platelets can aid and possibly initiate the progression of various vascular diseases. Throughout this overview, we will highlight both the historical investigations into the role of platelets in health and disease as well as some of the more current work. Overall, the authors aim for the readers to gain an appreciation for the complexity of platelet functions and the multifaceted role of platelets in the vascular system. © 2017 American Physiological Society. Compr Physiol 8:1117-1156, 2018.

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Prostacyclin inhibits platelet aggregation induced by phorbol ester or Ca2+ ionophore at steps distal to activation of protein kinase C and Ca2+-dependent protein kinases

Cited by 44 publications

References 52 publications

Translocation-independent activation of protein kinase C by platelet-activating factor, thrombin and prostacyclin. Lack of correlation with polyphosphoinositide hydrolysis in rabbit platelets

Translocation-independent activation of protein kinase C by platelet-activating factor, thrombin and prostacyclin. Lack of correlation with polyphosphoinositide hydrolysis in rabbit platelets

Prostacyclin and Sodium Nitroprusside Inhibit the Activity of the Platelet Inositol 1,4,5-Trisphosphate Receptor and Promote Its Phosphorylation

Platelet‐Activation Mechanisms and Vascular Remodeling

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