Dihydropyridine Agonist Bay K 8644 Inhibits Platelet Activation by Competitive Antagonism of Thromboxane A2-Prostaglandin H2 Receptor

The dihydropyridine calcium channel antagonists, such as nifedipine, inhibit platelet aggregation in vitro and ex vivo, but the mechanism by which this occurs is uncertain. Bay K 8644 (BAY) is a substituted dihydropyridine that has effects on voltage-dependent calcium channels in cardiac and smooth...

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Veröffentlicht in:	Circulation research 1988-03, Vol.62 (3), p.494-505
Hauptverfasser:	Johnson, Gerhard J, Dunlop, Patricia C, Leis, Linda A, From, Arthur H.L
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Sprache:	eng
Schlagworte:	3-Pyridinecarboxylic acid, 1,4-dihydro-2,6-dimethyl-5-nitro-4-(2-(trifluoromethyl)phenyl)-, Methyl ester - pharmacology Biological and medical sciences Blood. Blood coagulation. Reticuloendothelial system Humans In Vitro Techniques Ion Channels - drug effects Medical sciences Pharmacology. Drug treatments Platelet Aggregation - drug effects Prostaglandin Endoperoxides - metabolism Prostaglandins H - metabolism Receptors, Prostaglandin - drug effects Receptors, Thromboxane Receptors, Thromboxane A2, Prostaglandin H2 Thromboxane A2 - metabolism Thromboxanes - metabolism
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creator	Johnson, Gerhard J Dunlop, Patricia C Leis, Linda A From, Arthur H.L
description	The dihydropyridine calcium channel antagonists, such as nifedipine, inhibit platelet aggregation in vitro and ex vivo, but the mechanism by which this occurs is uncertain. Bay K 8644 (BAY) is a substituted dihydropyridine that has effects on voltage-dependent calcium channels in cardiac and smooth muscle that are opposite the effects of nifedipine. To evaluate the mechanism responsible for dihydropyridine-induced inhibition of platelet function, we studied the in vitro effects of BAY on human platelet aggregation and secretion plus several related biochemical parameters, including cytoplasmic ionized calcium ([Ca]1). BAY exerted concentration-dependent effects on platelet aggregation and secretion of [C] serotonin. BAY (1–10 μm) inhibited the second wave of platelet aggregation and secretion stimulated by adenosine diphosphate or epinephrine and blocked shape change, aggregation, and secretion induced by the thromboxane A2(TXA2) mimic, U46619. BAY also inhibited U46619-induced phosphorylation of the −40,000-dalton cytoplasmic protein substrate of protein kinase C (40K protein), formation of TXA2, and rise in [Ca]1, all biochemical consequences of platelet activation. The (+)-(R) enantiomer of BAY [BAY(+)] was predominantly responsible for the inhibitory effects of racemic BAY. Nifedipine had the same inhibitory effects on platelet function and biochemistry, except it was −10 times less potent than BAY. Since these results suggested inhibition of the TXA2-prostaglandin H2 (PGH2) receptor, we measured binding of [H]U46619 to intact platelets. BAY, BAY(+), and nifedipine all functioned as competitive antagonists of [H]U46619 binding (BAY K1 = 1.47 μM). They did not inhibit binding of [H]yohimbine to platelet α2-adrenergic receptors. At 1–10 nM BAY, BAY(+) and the (-)-(S) enantiomer of BAY [BAY(-)] all resulted in slight stimulation of platelet function and biochemical events. No significant increase in [H]U46619 binding was demonstrable, however. Therefore, dihydropyridines that function as either calcium channel agonists or antagonists in cardiac or smooth muscle exert concentration-dependent effects on platelet function. In nanomolar concentrations, they augment, and in micromolar concentrations, they inhibit platelet activation induced by TXA2 or U46619. These data indicate that dihydropyridines do not inhibit TXA2-induced platelet activation by an effect on voltage-dependent calcium channels; they define the mechanism of inhibition as competitive antagon
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Bay K 8644 (BAY) is a substituted dihydropyridine that has effects on voltage-dependent calcium channels in cardiac and smooth muscle that are opposite the effects of nifedipine. To evaluate the mechanism responsible for dihydropyridine-induced inhibition of platelet function, we studied the in vitro effects of BAY on human platelet aggregation and secretion plus several related biochemical parameters, including cytoplasmic ionized calcium ([Ca]1). BAY exerted concentration-dependent effects on platelet aggregation and secretion of [C] serotonin. BAY (1–10 μm) inhibited the second wave of platelet aggregation and secretion stimulated by adenosine diphosphate or epinephrine and blocked shape change, aggregation, and secretion induced by the thromboxane A2(TXA2) mimic, U46619. BAY also inhibited U46619-induced phosphorylation of the −40,000-dalton cytoplasmic protein substrate of protein kinase C (40K protein), formation of TXA2, and rise in [Ca]1, all biochemical consequences of platelet activation. The (+)-(R) enantiomer of BAY [BAY(+)] was predominantly responsible for the inhibitory effects of racemic BAY. Nifedipine had the same inhibitory effects on platelet function and biochemistry, except it was −10 times less potent than BAY. Since these results suggested inhibition of the TXA2-prostaglandin H2 (PGH2) receptor, we measured binding of [H]U46619 to intact platelets. BAY, BAY(+), and nifedipine all functioned as competitive antagonists of [H]U46619 binding (BAY K1 = 1.47 μM). They did not inhibit binding of [H]yohimbine to platelet α2-adrenergic receptors. At 1–10 nM BAY, BAY(+) and the (-)-(S) enantiomer of BAY [BAY(-)] all resulted in slight stimulation of platelet function and biochemical events. No significant increase in [H]U46619 binding was demonstrable, however. Therefore, dihydropyridines that function as either calcium channel agonists or antagonists in cardiac or smooth muscle exert concentration-dependent effects on platelet function. In nanomolar concentrations, they augment, and in micromolar concentrations, they inhibit platelet activation induced by TXA2 or U46619. These data indicate that dihydropyridines do not inhibit TXA2-induced platelet activation by an effect on voltage-dependent calcium channels; they define the mechanism of inhibition as competitive antagonism of the TXA2-PGH2 receptor. The mechanism responsible for augmentation of platelet activation is uncertain. The inhibitory effects of the antagonist dihydropyridines on platelet TXA2-PGH2 receptors suggest that they may exert similar effects on vascular TXA2-PGH2 receptors.</description><identifier>ISSN: 0009-7330</identifier><identifier>EISSN: 1524-4571</identifier><identifier>DOI: 10.1161/01.RES.62.3.494</identifier><identifier>PMID: 2449295</identifier><identifier>CODEN: CIRUAL</identifier><language>eng</language><publisher>Hagerstown, MD: American Heart Association, Inc</publisher><subject>3-Pyridinecarboxylic acid, 1,4-dihydro-2,6-dimethyl-5-nitro-4-(2-(trifluoromethyl)phenyl)-, Methyl ester - pharmacology ; Biological and medical sciences ; Blood. Blood coagulation. Reticuloendothelial system ; Humans ; In Vitro Techniques ; Ion Channels - drug effects ; Medical sciences ; Pharmacology. Drug treatments ; Platelet Aggregation - drug effects ; Prostaglandin Endoperoxides - metabolism ; Prostaglandins H - metabolism ; Receptors, Prostaglandin - drug effects ; Receptors, Thromboxane ; Receptors, Thromboxane A2, Prostaglandin H2 ; Thromboxane A2 - metabolism ; Thromboxanes - metabolism</subject><ispartof>Circulation research, 1988-03, Vol.62 (3), p.494-505</ispartof><rights>1988 American Heart Association, Inc.</rights><rights>1988 INIST-CNRS</rights><lds50>peer_reviewed</lds50><oa>free_for_read</oa><woscitedreferencessubscribed>false</woscitedreferencessubscribed><citedby>FETCH-LOGICAL-c2900-ce5d935858c8c9f18baf26dfe3522c712bb2ff9037bb35751c8db63ccf3a30593</citedby></display><links><openurl>$$Topenurl_article</openurl><openurlfulltext>$$Topenurlfull_article</openurlfulltext><thumbnail>$$Tsyndetics_thumb_exl</thumbnail><link.rule.ids>314,776,780,3674,27901,27902</link.rule.ids><backlink>$$Uhttp://pascal-francis.inist.fr/vibad/index.php?action=getRecordDetail&idt=7749489$$DView record in Pascal Francis$$Hfree_for_read</backlink><backlink>$$Uhttps://www.ncbi.nlm.nih.gov/pubmed/2449295$$D View this record in MEDLINE/PubMed$$Hfree_for_read</backlink></links><search><creatorcontrib>Johnson, Gerhard J</creatorcontrib><creatorcontrib>Dunlop, Patricia C</creatorcontrib><creatorcontrib>Leis, Linda A</creatorcontrib><creatorcontrib>From, Arthur H.L</creatorcontrib><title>Dihydropyridine Agonist Bay K 8644 Inhibits Platelet Activation by Competitive Antagonism of Thromboxane A2-Prostaglandin H2 Receptor</title><title>Circulation research</title><addtitle>Circ Res</addtitle><description>The dihydropyridine calcium channel antagonists, such as nifedipine, inhibit platelet aggregation in vitro and ex vivo, but the mechanism by which this occurs is uncertain. Bay K 8644 (BAY) is a substituted dihydropyridine that has effects on voltage-dependent calcium channels in cardiac and smooth muscle that are opposite the effects of nifedipine. To evaluate the mechanism responsible for dihydropyridine-induced inhibition of platelet function, we studied the in vitro effects of BAY on human platelet aggregation and secretion plus several related biochemical parameters, including cytoplasmic ionized calcium ([Ca]1). BAY exerted concentration-dependent effects on platelet aggregation and secretion of [C] serotonin. BAY (1–10 μm) inhibited the second wave of platelet aggregation and secretion stimulated by adenosine diphosphate or epinephrine and blocked shape change, aggregation, and secretion induced by the thromboxane A2(TXA2) mimic, U46619. BAY also inhibited U46619-induced phosphorylation of the −40,000-dalton cytoplasmic protein substrate of protein kinase C (40K protein), formation of TXA2, and rise in [Ca]1, all biochemical consequences of platelet activation. The (+)-(R) enantiomer of BAY [BAY(+)] was predominantly responsible for the inhibitory effects of racemic BAY. Nifedipine had the same inhibitory effects on platelet function and biochemistry, except it was −10 times less potent than BAY. Since these results suggested inhibition of the TXA2-prostaglandin H2 (PGH2) receptor, we measured binding of [H]U46619 to intact platelets. BAY, BAY(+), and nifedipine all functioned as competitive antagonists of [H]U46619 binding (BAY K1 = 1.47 μM). They did not inhibit binding of [H]yohimbine to platelet α2-adrenergic receptors. At 1–10 nM BAY, BAY(+) and the (-)-(S) enantiomer of BAY [BAY(-)] all resulted in slight stimulation of platelet function and biochemical events. No significant increase in [H]U46619 binding was demonstrable, however. Therefore, dihydropyridines that function as either calcium channel agonists or antagonists in cardiac or smooth muscle exert concentration-dependent effects on platelet function. In nanomolar concentrations, they augment, and in micromolar concentrations, they inhibit platelet activation induced by TXA2 or U46619. These data indicate that dihydropyridines do not inhibit TXA2-induced platelet activation by an effect on voltage-dependent calcium channels; they define the mechanism of inhibition as competitive antagonism of the TXA2-PGH2 receptor. The mechanism responsible for augmentation of platelet activation is uncertain. The inhibitory effects of the antagonist dihydropyridines on platelet TXA2-PGH2 receptors suggest that they may exert similar effects on vascular TXA2-PGH2 receptors.</description><subject>3-Pyridinecarboxylic acid, 1,4-dihydro-2,6-dimethyl-5-nitro-4-(2-(trifluoromethyl)phenyl)-, Methyl ester - pharmacology</subject><subject>Biological and medical sciences</subject><subject>Blood. Blood coagulation. Reticuloendothelial system</subject><subject>Humans</subject><subject>In Vitro Techniques</subject><subject>Ion Channels - drug effects</subject><subject>Medical sciences</subject><subject>Pharmacology. Drug treatments</subject><subject>Platelet Aggregation - drug effects</subject><subject>Prostaglandin Endoperoxides - metabolism</subject><subject>Prostaglandins H - metabolism</subject><subject>Receptors, Prostaglandin - drug effects</subject><subject>Receptors, Thromboxane</subject><subject>Receptors, Thromboxane A2, Prostaglandin H2</subject><subject>Thromboxane A2 - metabolism</subject><subject>Thromboxanes - metabolism</subject><issn>0009-7330</issn><issn>1524-4571</issn><fulltext>true</fulltext><rsrctype>article</rsrctype><creationdate>1988</creationdate><recordtype>article</recordtype><sourceid>EIF</sourceid><recordid>eNo9kc-P1CAcxYnRrOPq2ZMJB-OtXX61heM4ru7GTdys65kABYu2pQLj2j_A_1vGmeyBQHjv-3j5AMBrjGqMW3yBcH13-bVuSU1rJtgTsMENYRVrOvwUbBBCouooRc_Bi5R-IIQZJeIMnBHGBBHNBvz94Ie1j2FZo-_9bOH2e5h9yvC9WuFnyFvG4PU8eO1zgrejyna0GW5N9r9V9mGGeoW7MC02-3JVxues_idMMDh4P8Qw6fBHHYJJdRtDKvKo5vIUvCLwzhq75BBfgmdOjcm-Ou3n4NvHy_vdVXXz5dP1bntTGSIQqoxtekEb3nDDjXCYa-VI2ztLG0JMh4nWxDmBaKc1bboGG97rlhrjqKKoEfQcvDvmLjH82tuU5eSTsWNpZMM-yY5jxBjBxXhxNJpSOUXr5BL9pOIqMZIH8BJhWcDLlkgqC_gy8eYUvdeT7R_9J9JFf3vSVTJqdFHNxqdHW9eVEH5oyI62hzBmG9PPcf9goxysGvMgy38iijCpsOC8nAqTsjCi_wC4pJuC</recordid><startdate>198803</startdate><enddate>198803</enddate><creator>Johnson, Gerhard J</creator><creator>Dunlop, Patricia C</creator><creator>Leis, Linda A</creator><creator>From, Arthur H.L</creator><general>American Heart Association, Inc</general><general>Lippincott</general><scope>IQODW</scope><scope>CGR</scope><scope>CUY</scope><scope>CVF</scope><scope>ECM</scope><scope>EIF</scope><scope>NPM</scope><scope>AAYXX</scope><scope>CITATION</scope><scope>7X8</scope></search><sort><creationdate>198803</creationdate><title>Dihydropyridine Agonist Bay K 8644 Inhibits Platelet Activation by Competitive Antagonism of Thromboxane A2-Prostaglandin H2 Receptor</title><author>Johnson, Gerhard J ; Dunlop, Patricia C ; Leis, Linda A ; From, Arthur H.L</author></sort><facets><frbrtype>5</frbrtype><frbrgroupid>cdi_FETCH-LOGICAL-c2900-ce5d935858c8c9f18baf26dfe3522c712bb2ff9037bb35751c8db63ccf3a30593</frbrgroupid><rsrctype>articles</rsrctype><prefilter>articles</prefilter><language>eng</language><creationdate>1988</creationdate><topic>3-Pyridinecarboxylic acid, 1,4-dihydro-2,6-dimethyl-5-nitro-4-(2-(trifluoromethyl)phenyl)-, Methyl ester - pharmacology</topic><topic>Biological and medical sciences</topic><topic>Blood. Blood coagulation. Reticuloendothelial system</topic><topic>Humans</topic><topic>In Vitro Techniques</topic><topic>Ion Channels - drug effects</topic><topic>Medical sciences</topic><topic>Pharmacology. Drug treatments</topic><topic>Platelet Aggregation - drug effects</topic><topic>Prostaglandin Endoperoxides - metabolism</topic><topic>Prostaglandins H - metabolism</topic><topic>Receptors, Prostaglandin - drug effects</topic><topic>Receptors, Thromboxane</topic><topic>Receptors, Thromboxane A2, Prostaglandin H2</topic><topic>Thromboxane A2 - metabolism</topic><topic>Thromboxanes - metabolism</topic><toplevel>peer_reviewed</toplevel><toplevel>online_resources</toplevel><creatorcontrib>Johnson, Gerhard J</creatorcontrib><creatorcontrib>Dunlop, Patricia C</creatorcontrib><creatorcontrib>Leis, Linda A</creatorcontrib><creatorcontrib>From, Arthur H.L</creatorcontrib><collection>Pascal-Francis</collection><collection>Medline</collection><collection>MEDLINE</collection><collection>MEDLINE (Ovid)</collection><collection>MEDLINE</collection><collection>MEDLINE</collection><collection>PubMed</collection><collection>CrossRef</collection><collection>MEDLINE - Academic</collection><jtitle>Circulation research</jtitle></facets><delivery><delcategory>Remote Search Resource</delcategory><fulltext>fulltext</fulltext></delivery><addata><au>Johnson, Gerhard J</au><au>Dunlop, Patricia C</au><au>Leis, Linda A</au><au>From, Arthur H.L</au><format>journal</format><genre>article</genre><ristype>JOUR</ristype><atitle>Dihydropyridine Agonist Bay K 8644 Inhibits Platelet Activation by Competitive Antagonism of Thromboxane A2-Prostaglandin H2 Receptor</atitle><jtitle>Circulation research</jtitle><addtitle>Circ Res</addtitle><date>1988-03</date><risdate>1988</risdate><volume>62</volume><issue>3</issue><spage>494</spage><epage>505</epage><pages>494-505</pages><issn>0009-7330</issn><eissn>1524-4571</eissn><coden>CIRUAL</coden><abstract>The dihydropyridine calcium channel antagonists, such as nifedipine, inhibit platelet aggregation in vitro and ex vivo, but the mechanism by which this occurs is uncertain. Bay K 8644 (BAY) is a substituted dihydropyridine that has effects on voltage-dependent calcium channels in cardiac and smooth muscle that are opposite the effects of nifedipine. To evaluate the mechanism responsible for dihydropyridine-induced inhibition of platelet function, we studied the in vitro effects of BAY on human platelet aggregation and secretion plus several related biochemical parameters, including cytoplasmic ionized calcium ([Ca]1). BAY exerted concentration-dependent effects on platelet aggregation and secretion of [C] serotonin. BAY (1–10 μm) inhibited the second wave of platelet aggregation and secretion stimulated by adenosine diphosphate or epinephrine and blocked shape change, aggregation, and secretion induced by the thromboxane A2(TXA2) mimic, U46619. BAY also inhibited U46619-induced phosphorylation of the −40,000-dalton cytoplasmic protein substrate of protein kinase C (40K protein), formation of TXA2, and rise in [Ca]1, all biochemical consequences of platelet activation. The (+)-(R) enantiomer of BAY [BAY(+)] was predominantly responsible for the inhibitory effects of racemic BAY. Nifedipine had the same inhibitory effects on platelet function and biochemistry, except it was −10 times less potent than BAY. Since these results suggested inhibition of the TXA2-prostaglandin H2 (PGH2) receptor, we measured binding of [H]U46619 to intact platelets. BAY, BAY(+), and nifedipine all functioned as competitive antagonists of [H]U46619 binding (BAY K1 = 1.47 μM). They did not inhibit binding of [H]yohimbine to platelet α2-adrenergic receptors. At 1–10 nM BAY, BAY(+) and the (-)-(S) enantiomer of BAY [BAY(-)] all resulted in slight stimulation of platelet function and biochemical events. No significant increase in [H]U46619 binding was demonstrable, however. Therefore, dihydropyridines that function as either calcium channel agonists or antagonists in cardiac or smooth muscle exert concentration-dependent effects on platelet function. In nanomolar concentrations, they augment, and in micromolar concentrations, they inhibit platelet activation induced by TXA2 or U46619. These data indicate that dihydropyridines do not inhibit TXA2-induced platelet activation by an effect on voltage-dependent calcium channels; they define the mechanism of inhibition as competitive antagonism of the TXA2-PGH2 receptor. The mechanism responsible for augmentation of platelet activation is uncertain. The inhibitory effects of the antagonist dihydropyridines on platelet TXA2-PGH2 receptors suggest that they may exert similar effects on vascular TXA2-PGH2 receptors.</abstract><cop>Hagerstown, MD</cop><pub>American Heart Association, Inc</pub><pmid>2449295</pmid><doi>10.1161/01.RES.62.3.494</doi><tpages>12</tpages><oa>free_for_read</oa></addata></record>
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source	MEDLINE; American Heart Association Journals; Elektronische Zeitschriftenbibliothek - Frei zugängliche E-Journals; Journals@Ovid Complete
subjects	3-Pyridinecarboxylic acid, 1,4-dihydro-2,6-dimethyl-5-nitro-4-(2-(trifluoromethyl)phenyl)-, Methyl ester - pharmacology Biological and medical sciences Blood. Blood coagulation. Reticuloendothelial system Humans In Vitro Techniques Ion Channels - drug effects Medical sciences Pharmacology. Drug treatments Platelet Aggregation - drug effects Prostaglandin Endoperoxides - metabolism Prostaglandins H - metabolism Receptors, Prostaglandin - drug effects Receptors, Thromboxane Receptors, Thromboxane A2, Prostaglandin H2 Thromboxane A2 - metabolism Thromboxanes - metabolism
title	Dihydropyridine Agonist Bay K 8644 Inhibits Platelet Activation by Competitive Antagonism of Thromboxane A2-Prostaglandin H2 Receptor
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