In the presence of strong P2Y12 receptor blockade, aspirin provides little additional inhibition of platelet aggregation

Armstrong, Paul C; Leadbeater, P. D. M.; Chan, Melissa; Kirkby, Nicholas S.; Jakubowski, Joseph A.; Mitchell, Jane A.; Warner, Timothy D.

doi:10.1111/j.1538-7836.2010.04160.x

Cited by 168 publications

(125 citation statements)

References 41 publications

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“…As we have previously reported in standard 96-well plate and optimul kinetic aggregometry [1,[4][5][6], we found that aspirin significantly inhibited ( p < 0.05) aggregation induced by EPI and completely abolished responses to AA and collagen. PAM, however, significantly attenuated ( p < 0.05) aggregation induced by all agonists tested, except for ristocetin, which acts through a process that involves agglutination and not aggregation.…”

supporting

confidence: 84%

Standardised optical multichannel (optimul) platelet aggregometry using high-speed shaking and fixed time point readings

Chan

Warner

2011

Platelets

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supporting

confidence: 84%

Standardised optical multichannel (optimul) platelet aggregometry using high-speed shaking and fixed time point readings

Chan

Warner

2011

Platelets

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“…In particular, the level of platelet inhibition achieved by combining aspirin and a potent P2Y 12 receptor antagonist is no greater than that produced by the P2Y 12 receptor antagonist alone. 31 Our study confirms these in vitro findings by demonstrating in vivo that potent P2Y 12 receptor blockade with both prasugrel and ticagrelor is also associated with inhibitory effects on measures of non-ADP-induced platelet reactivity. In particular, our study further expands on previous observations showing that, in DM patients, the addition of either prasugrel or ticagrelor on top of aspirin is able to significantly reduce thromboxane A 2 -mediated platelet reactivity, as assessed by assays sensitive to aspirin-induced effects (arachidonic acid-and collageninduced aggregation), and platelet reactivity mediated by thrombin, as well, in both the acute and maintenance phases of treatment.…”

supporting

confidence: 78%

Pharmacodynamic Comparison of Prasugrel Versus Ticagrelor in Patients With Type 2 Diabetes Mellitus and Coronary Artery Disease

et al. 2016

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BACKGROUND:Patients with diabetes mellitus (DM) are at increased risk of atherothrombotic events, underscoring the importance of effective platelet inhibiting therapies. Prasugrel and ticagrelor reduce thrombotic complications to a greater extent than clopidogrel. Subgroup analyses of pivotal clinical trials testing prasugrel and ticagrelor versus clopidogrel showed DM patients to have benefits that were consistent with the overall trial populations, although the magnitude of the ischemic risk reduction appeared to be enhanced with prasugrel. Whether these findings may be attributed to differences in the pharmacodynamic profiles of these drugs in DM patients remains poorly explored and represented the aim of this study. METHODS:In this prospective, randomized, double-blind, double-dummy, crossover pharmacodynamic study, aspirin-treated DM patients (n=50) with coronary artery disease were randomly assigned to receive prasugrel (60 mg loading dose [LD]/10 mg maintenance dose once daily) or ticagrelor (180 mg LD/90 mg maintenance dose twice daily) for 1 week. Pharmacodynamic assessments were conducted using 4 different assays, including VerifyNow P2Y12, vasodilator-stimulated phosphoprotein, light transmittance aggregometry, and Multiplate, which allowed us to explore ADP-and non-ADP-induced (arachidonic acid-, collagen-, thrombin receptor-activating, peptide-induced) platelet signaling pathways. The acute (baseline, 30 minutes, and 2 hours post-LD) and maintenance (1 week) effects of therapy were assessed. The primary end point of the study was the comparison of P2Y 12 reaction units determined by VerifyNow P2Y12 at 1 week between prasugrel and ticagrelor.RESULTS: ADP-and non-ADP-induced measures of platelet reactivity reduced significantly with both prasugrel and ticagrelor LD and maintenance dose. P2Y 12 reaction units defined by VerifyNow were similar between prasugrel and ticagrelor at 30 minutes and 2 hours post-LD. At 1 week, P2Y 12 reaction units were significantly lower with ticagrelor than with prasugrel (52 [32-72] versus 83 [63-103]; least-square means difference: -31; 95% confidence interval, -57 to -4; P=0.022; primary end point). Pharmacodynamic assessments measured by vasodilator-stimulated phosphoprotein, light transmittance aggregometry, and Multiplate were similar between prasugrel and ticagrelor at each time point, including at 1 week. Rates of high on-treatment platelet reactivity were similar between groups with all assays at all time points. CONCLUSIONS:In DM patients with coronary artery disease, ticagrelor exerts similar or greater inhibition of ADP-induced platelet reactivity in comparison with prasugrel in the acute and chronic phases of treatment, whereas the inhibition of measures of non-ADP-induced platelet reactivity was not significantly different between the 2 agents.

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“…The effects of aspirin on platelet reactivity are relatively limited compared with P2Y 12 inhibition. 13 Furthermore, it has been suggested that P2Y 12 inhibition alone may partially inhibit platelet thromboxane A 2 synthesis, 14,15 and in the presence of strong P2Y 12 inhibition, the additional effects of higher aspirin doses may result in a reduction of prostacyclin release, potentially shifting the influence of aspirin to a prothrombotic effect. 16 Consistent with the Clopidogrel Optimal Loading Dose Usage to Reduce Recurrent Events/Optimal Antiplatelet Strategy for Interventions (CURRENT/OASIS 7) trial, 17 no association of aspirin maintenance dose with ischemic event rates in the clopidogrel group was observed.…”

Section: Discussionmentioning

confidence: 99%

Ticagrelor Compared With Clopidogrel by Geographic Region in the Platelet Inhibition and Patient Outcomes (PLATO) Trial

et al. 2011

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on behalf of the PLATO Investigators Background-In the Platelet Inhibition and Patient Outcomes (PLATO) trial, a prespecified subgroup analysis showed a significant interaction between treatment and region (Pϭ0.045), with less effect of ticagrelor in North America than in the rest of the world. Methods and Results-Reasons for the interaction were explored independently by 2 statistical groups. Systematic errors in trial conduct were investigated. Statistical approaches evaluated the likelihood of play of chance. Cox regression analyses were performed to quantify how much of the regional interaction could be explained by patient characteristics and concomitant treatments, including aspirin maintenance therapy. Landmark Cox regressions at 8 time points evaluated the association of selected factors, including aspirin dose, with outcomes by treatment. Systematic errors in trial conduct were ruled out. Given the large number of subgroup analyses performed and that a result numerically favoring clopidogrel in at least 1 of the 4 prespecified regions could occur with 32% probability, chance alone cannot be ruled out. More patients in the United States (53.6%) than in the rest of the world (1.7%) took a median aspirin dose Ն300 mg/d. Of 37 baseline and postrandomization factors explored, only aspirin dose explained a substantial fraction of the regional interaction. In adjusted analyses, both Cox regression with median maintenance dose and landmark techniques showed that, in patients taking low-dose maintenance aspirin, ticagrelor was associated with better outcomes compared with clopidogrel, with statistical superiority in the rest of the world and similar outcomes in the US cohort. Conclusions-The regional interaction could arise from chance alone. Results of 2 independently performed analyses identified an underlying statistical interaction with aspirin maintenance dose as a possible explanation for the regional difference. The lowest risk of cardiovascular death, myocardial infarction, or stroke with ticagrelor compared with clopidogrel is associated with a low maintenance dose of concomitant aspirin. Clinical Trial Registration-URL: http://www.clinicaltrials.gov. Unique identifier: NCT00391872. (Circulation. 2011;124:544-554.)

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In the presence of strong P2Y12 receptor blockade, aspirin provides little additional inhibition of platelet aggregation

Cited by 168 publications

References 41 publications

Standardised optical multichannel (optimul) platelet aggregometry using high-speed shaking and fixed time point readings

Standardised optical multichannel (optimul) platelet aggregometry using high-speed shaking and fixed time point readings

Pharmacodynamic Comparison of Prasugrel Versus Ticagrelor in Patients With Type 2 Diabetes Mellitus and Coronary Artery Disease

Ticagrelor Compared With Clopidogrel by Geographic Region in the Platelet Inhibition and Patient Outcomes (PLATO) Trial

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