1998
DOI: 10.1073/pnas.95.14.8070
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Coactivation of two different G protein-coupled receptors is essential for ADP-induced platelet aggregation

Abstract: ADP is an important platelet agonist causing shape change and aggregation required for physiological hemostasis. We recently demonstrated the existence of two distinct G protein-coupled ADP receptors on platelets, one coupled to phospholipase C, P2Y1, and the other to inhibition of adenylyl cyclase, P2T AC . In this study, using specific antagonists for these two receptors, we demonstrated that concomitant intracellular signaling from both the P2T AC and P2Y1 receptors is essential for ADP-induced platelet agg… Show more

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Cited by 494 publications
(474 citation statements)
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“…ADP binds to the G‐protein‐coupled receptors P2Y 1 22 and P2Y 12 23, 24 located on the platelet surface membrane. For a normal ADP‐induced activation and aggregation, responses from both pathways are required 25, 26, 27. When a P2Y 12 ‐receptor antagonist such as ticagrelor has bound to the platelet receptor, the ADP‐induced activation of P2Y 12 is inhibited.…”
Section: Discussionmentioning
confidence: 99%
See 1 more Smart Citation
“…ADP binds to the G‐protein‐coupled receptors P2Y 1 22 and P2Y 12 23, 24 located on the platelet surface membrane. For a normal ADP‐induced activation and aggregation, responses from both pathways are required 25, 26, 27. When a P2Y 12 ‐receptor antagonist such as ticagrelor has bound to the platelet receptor, the ADP‐induced activation of P2Y 12 is inhibited.…”
Section: Discussionmentioning
confidence: 99%
“…When a P2Y 12 ‐receptor antagonist such as ticagrelor has bound to the platelet receptor, the ADP‐induced activation of P2Y 12 is inhibited. Adrenaline binds to the α 2A ‐receptor, activating a pathway which mimics the P2Y 12 ‐receptor mediated pathway 26, 28, 29. This may explain that the combination of addition of ADP and adrenaline to blood samples from patients on ongoing treatment with ticagrelor results in a better aggregation response compared to either substance alone, as responses from both signaling pathways are achieved.…”
Section: Discussionmentioning
confidence: 99%
“…Co-activation of the P2Y 1 and P2Y 12 receptors is necessary for normal ADP-induced platelet aggregation since separate inhibition of either of them with selective antagonists results in a dramatic decrease in aggregation [22,46,80]. The P2Y 1 and P2Y 12 receptors are differentially involved in platelet aggregation induced by other agonists, with the P2Y 1 playing only a minor role, except in the case of collagen-induced activation, while P2Y 12 supports amplification of these responses.…”
Section: Receptormentioning
confidence: 99%
“…Similarly, the ADP receptor P2Y1, which is not very abundant on the platelet surface[19], is rapidly desensitized[20,21]. Thus, it can only cause a rapid but short-lived rise of the cytosolic calcium concentration and needs co-signaling through the P2Y12 receptor to support platelet aggregation[22,23]. So both PAR1 and P2Y1 are very sensitive and provide a fast but reversible activation response, while PAR4 and P2Y12 are required to sustain the signal.…”
Section: Classical Hemostasis – Balancing Platelet Adhesiveness In CImentioning
confidence: 99%