2000
DOI: 10.1055/s-0037-1614049
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Desensitization of the Platelet Aggregation Response to ADP: Differential Down-regulation of the P2Y1 and P2cyc Receptors

Abstract: SummaryPlatelets activated by ADP become refractory to restimulation, but the mechanism of this process is not well understood. A normal platelet response to ADP requires coactivation of the P2Y1 receptor responsible for shape change and the P2cyc receptor, responsible for completion and amplification of the response. The aim of the present study was to characterize the desensitization of platelets to ADP and to determine whether or not these two receptors are desensitized simultaneously through identical path… Show more

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Cited by 121 publications
(140 citation statements)
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“…The molecular mechanisms of this phenomenon have been studied in detail, but consensus has not been reached, and two different views have not yet been reconciled. On the one hand, it is thought that the phenomenon of platelet refractoriness to ADP is due to selective desensitization and internalization of the P2Y 1 receptor, while the P2Y 12 receptor remains functional with the ability of ADP to induce amplification of the platelet aggregation induced by other agonists [89][90][91]. Desensitization of the P2Y 1 receptor has been shown to be dependent on receptor C-terminal phosphorylation sites, β-arrestin-2 interaction and protein kinase C (PKC) activity [92,93].…”
Section: Desensitizationmentioning
confidence: 99%
“…The molecular mechanisms of this phenomenon have been studied in detail, but consensus has not been reached, and two different views have not yet been reconciled. On the one hand, it is thought that the phenomenon of platelet refractoriness to ADP is due to selective desensitization and internalization of the P2Y 1 receptor, while the P2Y 12 receptor remains functional with the ability of ADP to induce amplification of the platelet aggregation induced by other agonists [89][90][91]. Desensitization of the P2Y 1 receptor has been shown to be dependent on receptor C-terminal phosphorylation sites, β-arrestin-2 interaction and protein kinase C (PKC) activity [92,93].…”
Section: Desensitizationmentioning
confidence: 99%
“…In contrast to previous studies of LPA-induced aggregation of isolated platelets, platelets in our study were washed in the presence of prostacyclin and resuspended in buffer containing apyrase to avoid platelet preactivation and desensitization of the ADP-receptor P2Y 1 . 23 In this preparation, 1-acyl-LPA (16:0) induced shape change and subsequent aggregation with an EC 50 of 8 M. A concentration of 1 M 1-acyl-LPA (16:0) only induced shape change, 3M 1-acyl-LPA (16:0) induced shape change, reversible aggregation (10%) with only 1% to 2% serotonin secretion, higher concentrations (10, 30, and 100 M ) 1-acyl-LPA [16:0]) elicited maximal irreversible aggregation with 9%, 19%, and 36% serotonin secretion, respectively (data not shown and Figure 2A). 1-alkyl-LPA (16:0) was again more potent than 1-acyl-LPA (16:0) in inducing shape change and aggregation of washed platelets (data not shown).…”
Section: Lpamentioning
confidence: 99%
“…In order to minimize inappropriate platelet recruitment and activation at the site of a growing thrombus, platelet ADP responsiveness is tightly regulated in human platelets (8)(9)(10)(11)(12). P2Y 12 receptor responsiveness rapidly desensitizes in human platelets (13).…”
Section: A C C E P T E D Accepted Manuscriptmentioning
confidence: 99%