cAMP reduces the affinity of Ca<sup>2+</sup>‐triggered secretion in platelets

Collazos, J.M.; Sánchez, Abraham

doi:10.1016/0014-5793(87)80138-2

Cited by 10 publications

(7 citation statements)

References 15 publications

(15 reference statements)

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“…The Ca2+-dependent phosphorylation of the 20 and 47 kDa proteins induced by ionophore A23187 was not inhibited by PGI2. In agreement with previous studies [10,33,34], aggregation but not shape change was inhibited by PGI2. Since Ca2+ mobilization induced by ionophore A23187 was not inhibited by PGI2 (see also refs.…”

Section: Discussionsupporting

confidence: 93%

“…Since Ca2+ mobilization induced by ionophore A23187 was not inhibited by PGI2 (see also refs. [33,34]), these results indicate that aggregation is inhibited by PGI2 at steps distal to Ca2+-dependent phosphorylation of 20 and 47 kDa proteins. This result is somewhat unexpected: biochemical studies using purified proteins have demonstrated that protein kinase A phosphorylates MLCK, thereby diminishing its enzymic activity and decreasing its affinity for calmodulin [4,37].…”

Section: Discussionmentioning

confidence: 67%

“…Different studies, however, have indicated that other target sites exist for cyclic AMP. For example, cyclic AMP inhibits Ca2+-dependent secretion and aggregation at steps distal to Ca2l mobilization [33][34][35][36]. Also, it has been reported that the catalytic subunit of cyclic AMPdependent kinase phosphorylates the purified Ca2"/ calmodulin-dependent MLCK, thereby decreasing its ability to phosphorylate myosin light chain [37].…”

Section: Introductionmentioning

confidence: 99%

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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

Siess

Lapetina

1989

Biochemical Journal

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Suspensions of aspirin-treated, 32P-prelabelled, washed platelets containing ADP scavengers in the buffer were activated with either phorbol 12,13-dibutyrate (PdBu) or the Ca2+ ionophore A23187. High concentrations of PdBu (greater than or equal to 50 nM) induced platelet aggregation and the protein kinase C (PKC)-dependent phosphorylation of proteins with molecular masses of 20 (myosin light chain), 38 and 47 kDa. No increase in cytosolic Ca2+ was observed. Preincubation of platelets with prostacyclin (PGI2) stimulated the phosphorylation of a 50 kDa protein [EC50 (concn. giving half-maximal effect) 0.6 ng of PGI2/ml] and completely abolished platelet aggregation [ID50 (concn. giving 50% inhibition) 0.5 ng of PGI2/ml] induced by PdBu, but had no effect on phosphorylation of the 20, 38 and 47 kDa proteins elicited by PdBu. The Ca2+ ionophore A23187 induced shape change, aggregation, mobilization of Ca2+, rapid phosphorylation of the 20 and 47 kDa proteins and the formation of phosphatidic acid. Preincubation of platelets with PGI2 (500 ng/ml) inhibited platelet aggregation, but not shape change, Ca2+ mobilization or the phosphorylation of the 20 and 47 kDa proteins induced by Ca2+ ionophore A23187. The results indicate that PGI2, through activation of cyclic AMP-dependent kinases, inhibits platelet aggregation at steps distal to protein phosphorylation evoked by protein kinase C and Ca2+-dependent protein kinases.

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Section: Discussionsupporting

confidence: 93%

Section: Discussionmentioning

confidence: 67%

Section: Introductionmentioning

confidence: 99%

See 1 more Smart Citation

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

Lapetina

1989

Biochemical Journal

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“…For this, cAMP activates a protein kinase that phosphorylates an ATP-dependent calcium-pump. Subsequently, Ca 2+ uptake into the dense tubular system is subsequently decreased, resulting in the inhibition of platelet activation cascades [83][84][85]. In the present study, we found that treatment with baicalein elevated the level of cAMP in resting platelets.…”

Section: Discussionmentioning

confidence: 65%

Baicalein inhibits agonist- and tumor cell-induced platelet aggregation while suppressing pulmonary tumor metastasis via cAMP-mediated VASP phosphorylation along with impaired MAPKs and PI3K-Akt activation

Kim¹,

Lee²,

Baik³

et al. 2014

Biochemical Pharmacology

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“…Other studies discovered additional target sites for platelet inhibition by cyclic AMP. For example, several investigators reported that cyclic AMP inhibits secretion and aggregation induced by Ca2+ ionophore at steps distal to Ca2l mobilization [6][7][8][9]. Also, modest increments in platelet cyclic AMP were reported to abolish platelet-activatingfactor-induced aggregation and secretion, whereas they had little effect on phosphoinositide hydrolysis and elevation of cytosolic Ca2+ concentration induced by platelet-activating factor [10].…”

Section: Introductionmentioning

confidence: 99%

Functional relationship between cyclic AMP-dependent protein phosphorylation and platelet inhibition

Siess

Lapetina

1990

Biochemical Journal

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Exposure of human platelets to prostacyclin (PGI2), iloprost or prostaglandin E1 (PGE1) elicits the cyclic AMP-dependent phosphorylation of proteins of 22, 24, 30, 39, 50, 60 and 250 kDa (P22, P24 etc.). P22 was recently identified as rap 1B, a ras-like protein, and P24 was shown to be the beta-chain of glycoprotein Ib. We found that cyclic AMP-dependent phosphorylation of all proteins except P22 was maximal 1 min after exposure of platelets to PGI2, iloprost or PGE1; maximal phosphorylation of P22 occurred after 45 min of incubation. Inhibition of thrombin-induced platelet activation required only a 30 s incubation with PGI2 or iloprost; at this time phosphorylation of P22 was only slightly increased. Although at maximal concentrations PGI2 was more potent than PGE1 in inhibiting thrombin-induced platelet activation, no difference in the degree and the kinetics of cyclic AMP-dependent protein phosphorylation was found. Platelets that had been preincubated and washed in the presence of PGE1 and later resuspended in the absence of PGE1 responded fully to activation by thrombin despite maximal phosphorylation of P22 and P24. Furthermore, addition of PGI2 to PGE1-washed platelets prevented thrombin-induced platelet activation, but did not evoke further phosphorylation of P22 or P24. Phosphorylation of P39 and P50 correlated better with PGI2-induced inhibition of platelet activation. In experiments in which PGE1-induced inhibition of platelet activation was overcome by the addition of thrombin, no dephosphorylation of proteins phosphorylated by cyclic AMP-dependent kinases was observed. These experiments indicate that: (a) phosphorylation of rap 1B and glycoprotein Ib is not related to platelet inhibition by cyclic AMP; (b) phosphorylation of other proteins such as P39 and P50 probably plays a role in mediating cyclic AMP-dependent platelet inhibition; (c) reactions other than cyclic AMP-dependent protein phosphorylation may participate in platelet inhibition by cyclic AMP.

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cAMP reduces the affinity of Ca²⁺‐triggered secretion in platelets

Cited by 10 publications

References 15 publications

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

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

Baicalein inhibits agonist- and tumor cell-induced platelet aggregation while suppressing pulmonary tumor metastasis via cAMP-mediated VASP phosphorylation along with impaired MAPKs and PI3K-Akt activation

Functional relationship between cyclic AMP-dependent protein phosphorylation and platelet inhibition

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cAMP reduces the affinity of Ca2+‐triggered secretion in platelets

Cited by 10 publications

References 15 publications

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

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

Baicalein inhibits agonist- and tumor cell-induced platelet aggregation while suppressing pulmonary tumor metastasis via cAMP-mediated VASP phosphorylation along with impaired MAPKs and PI3K-Akt activation

Functional relationship between cyclic AMP-dependent protein phosphorylation and platelet inhibition

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cAMP reduces the affinity of Ca²⁺‐triggered secretion in platelets