Measuring Platelet Reactivity after Clopidogrel-Has it Reached the End of the Road?

Wong, Cheuk Kit

doi:10.4172/2329-6607.1000e105

Cited by 6 publications

(16 citation statements)

References 17 publications

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“…Clopidogrel is a pro-drug requiring a 2-step hepatic activation processes. Speed of activation varies according to the cytochrome P-450 2C19 allele [1,2]. Ticagrelor is a direct non-thienopyridine P2Y12 antagonist producing equal or stronger inhibition of the P2Y12 receptor even when compared to the newer thienopyridine prasugrel [3].…”

Section: Editorialmentioning

confidence: 99%

Trials Evaluating Ticagrelor in Cardiovascular Disease: Will It Reign Supreme in the Anti-Platelet World?

Wong¹

2017

Cardiovasc Pharm Open Access

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EditorialTicagrelor and prasugrel are newer and stronger platelet P2Y12 receptor antagonists than their predecessor clopidogrel. Clopidogrel is a pro-drug requiring a 2-step hepatic activation processes. Speed of activation varies according to the cytochrome P-450 2C19 allele [1,2]. Ticagrelor is a direct non-thienopyridine P2Y12 antagonist producing equal or stronger inhibition of the P2Y12 receptor even when compared to the newer thienopyridine prasugrel [3]. The PLATO TrialIn the PLATO trial of 18624 patients with acute coronary syndrome on background aspirin therapy, ticagrelor 90 mg twice daily significantly reduced all-cause and cardiovascular mortality as compared to clopidogrel 75 mg daily (4.5% vs. 5.9% and 4.0% vs. 5.1% respectively over 1-year) [4]. In PLATO, the Kaplan-Meier curves showing the adjudicated primary end point (a composite of death from vascular causes, myocardial infarction, or stroke) separated in the first month and kept diverging throughout the year. These positive findings held true in the very large subgroup of patients with coronary stent implanted, and ticagrelor reduced stent thrombosis more as compared to clopidogrel [5]. Ticagrelor treated patients had higher nonprocedural but not CABG-related or fatal bleeding compared to clopidogrel treated patient [4], perhaps an expected finding given that ticagrelor is a stronger but reversible P2Y12 antagonist (with faster offset of action) while clopidogrel is a weaker but non-reversible P2Y12 antagonist.In PLATO a geographical regional interaction was noted (with interaction P value of 0.05) where outcome trended in opposite direction between patients randomized in North America (n=1814) and patients randomized elsewhere. In these 1814 patients, outcome tended to be worse with ticagrelor than with clopidogrel (HR 1.25, 95% CI 0.93-1.67). Exploratory analysis revealed only one factor-aspirin dose (higher in North America than elsewhere) that might explain the observed regional interaction [6]. Currently, the advantage from ticagrelor as compared with clopidogrel is believed to be associated only with the use of low-dose (<100 mg) aspirin, and guidelines specify this point. Dual antiplatelet therapy post coronary stentingPrevious editorials in the Journal have reviewed the basis for dual antiplatelet therapy post coronary stenting [1,2]. In a very recent patient level meta-analysis of 11,473 patients with coronary stenting (58.5% with stable coronary disease) from 6 randomized trials, patients with ≤6 month dual antiplatelet therapy tended to have higher 1-year event rates of myocardial infarction or stent thrombosis than patients with 1-year dual antiplatelet therapy (HR 1.48; 95% CI, 0.98-2.22) if they were stented for unstable disease; while rates were similar if they were stented for stable disease (HR 0.93; 95% CI, interaction P value=0.09). By network meta-analysis, 3-month but not 6-month dual antiplatelet therapy was associated with higher event rates in the former patients whereas no significant differences were apparent in the...

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Section: Editorialmentioning

confidence: 99%

Trials Evaluating Ticagrelor in Cardiovascular Disease: Will It Reign Supreme in the Anti-Platelet World?

Wong¹

2017

Cardiovasc Pharm Open Access

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“…Relevant CYP isoenzymes involved in activating clopidogrel (and to a lesser extent prasugrel) may be affected by genetic polymorphisms which lead to different levels of their final active metabolites binding irreversibly to the platelet P2Y 12 receptors. For clopidogrel, patients with either 1 or 2 loss-of-function CYP2C19 alleles are known to have an attenuated pharmacologic response and worse clinical outcomes, with greater impairment in those who had both alleles affected [3].…”

Section: Why Antarctic Failed and What Remains For Tailored Antiplatementioning

confidence: 99%

“…The situation is different with the use of clopidogrel for which up to 40% of patients are somewhat resistant [4] with the occasional patients (often having 2 loss-of-function CYP2C19 alleles) actually having minimal platelet suppression and potentially unduly high risks of stent thrombosis. The latter situation should be remedied by switching clopidogrel to prasugrel or ticagrelor [3].…”

Section: Why Antarctic Failed and What Remains For Tailored Antiplatementioning

confidence: 99%

“…The cut-points for determining high PRU were obtained from observational studies [3]. The ADAPT-DES registry supported the use of the PRU cut-point of 208 on the VerifyNow P2Y 12 cartridge platelet function test [4].…”

Section: Observational Studies and Randomized Trials-what Questions Rmentioning

confidence: 99%

“…An editorial in this journal commenting on ARCTIC questioned whether measuring platelet reactivity after clopidogrel could be reaching the end of the road [3], given that more efficacious antiplatelet medications such as prasugrel were becoming available. Indeed in ANTARCTIC, a "low" dose of prasugrel of 5 mg turned out to give sufficiently adequate platelet suppression in >96% of patients.…”

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confidence: 99%

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From Arctic to Antarctic: Is There any Remaining Role for Platelet Function Testing to Tailor Therapy after Coronary Stent Implantation?

Wong¹

2016

Cardiovasc Pharm Open Access

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EditorialOpen Access Cardiovascular Pharmacology: Open Access C a rd iovascu la r P h ar macol o g y : O pe n Acc es s ISSN: 2329-6607The recently reported ANTARCTIC trial [1] is an open-label, blinded endpoint-adjudication, randomised controlled superiority study from 35 centres in France testing the role of tailored antiplatelet therapy among 877 elderly patients (41% women and 28% diabetics) over the age of 75 years (~20% over 85) with either ST elevation or non-ST elevation acute myocardial infarction undergoing coronary stenting.Patients (recruited between March 2012 and May 2015) were started on prasugrel 5 mg daily and randomized to tailored antiplatelet therapy (n=435) versus conventional therapy (n=442). Platelet function was assessed by the point-of-care VerifyNow P2Y 12 cartridge platelet function test performed on days 14 and 28. If platelet reactivity unit (PRU) was ≥208, prasugrel was increased to 10 mg daily; and if ≤85, prasugrel was changed to clopidogrel 75 mg daily.The trial excluded patients with previous history of transient ischaemic attack or stroke, fibrinolytic therapy within the past 48 h, chronic oral anticoagulation, concomitant medical illness with reduced survival, allergy or intolerance to aspirin or thienopyridines, active bleeding or history of bleeding diathesis, thrombocytopenia, severe hepatic impairment, or conditions potentially associated with poor treatment adherence such as dementia.It turned out that in the tailored antiplatelet therapy group only 3.7% required escalation to prasugrel 10 mg daily while 39.3% were converted to clopidogrel 75 mg daily. The primary outcome, measuring the composite of cardiovascular death, myocardial infarction, stroke, stent thrombosis, urgent revascularization, or bleeding complication at 1 year, occurred in 27.6% of the tailored therapy group vs. 27.8% of the conventional therapy group (p=0.98). Secondary outcome measuring the composite of cardiovascular death, myocardial infarction, stent thrombosis, or urgent revascularization was also not different, 9.9% vs. 9.3% respectively (p=0.80).The ANTARCTIC authors concluded that platelet function monitoring with treatment adjustment did not improve clinical outcomes. They further remarked in their concluding paragraph of the abstract that "…..platelet function testing is being used in many centres and international guidelines still recommend platelet function testing in high-risk situations. Our study does not support this practice or these recommendations."Where Do We Stand with Anti-Platelet Therapy PostCoronary Stenting?The basis for dual antiplatelet agents (aspirin plus a P2Y 12 receptor antagonist) in preventing acute and sub-acute thrombosis after coronary stenting was established 2 decades ago. The era of drug eluting stents from the last decade onwards ushered the practice of prolonged dual antiplatelet therapy in the hope of preventing late stent thrombosis. With this approach comes the conundrum between antithrombotic benefit versus bleeding risk, hence the quest for a potential "sw...

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Time for a Reappraisal: How much has the Last 10 Years of Ã¢ÂÂMainstreamÃ¢ÂÂ STEMI Research Impacted on STEMI Outcome?

2015

Cardiol Pharmacol

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EditorialEvidenced based management of STEMI reperfusion is built on large-scale randomized trials with solid clinical endpoints. Promptly performed primary PCI, as measured by the door-to-balloon time within 90 minutes, is the current treatment standard. This key quality metric is tracked by many hospital databases, clinical registries etc., and is even made publicly available in some places.Funded by the National Cardiovascular Data Registry of the American College of Cardiology Foundation, an analysis of the Cath-PCI registry reported unchanged in-hospital mortality (both observed and risk-adjusted mortality) from July 2005 through June 2009 for STEMI despite significant shortened door-to-balloon time from 83 minutes to 67 minutes in America [1]. The authors suggested that additional strategies were needed to reduce mortality.A re-analysis of the same data by another group of investigators (adding at both ends of an extended period to include all complete years 2005 -2011) [2] "vindicated" the importance of door-to-balloon time showing the positive and almost linear relationship between door-to-balloon time and observed in-hospital mortality within every calendar year. However, for the same door-to-balloon time when it was over ~70 minutes, mortality was consistently higher in later years than in earlier years. The net effect combining all patients was that over the 7 years door-to-balloon time had shortened from ~90 to ~65 minutes but mortality had not declined. Risk-adjusted in-hospital mortality showed a trend of an increase (from 4·7% to 5·3%) and risk-adjusted 6-month mortality showed an increase from 12·9% to 14·4% (p=0·001) [2].Although more patients underwent PCI in later than in earlier years, there were only small variations in patient demographics. Their mean age was 61 years. To explain the paradoxical higher mortality over the more recent years among those patients with door-to balloon time over ~70 minutes, the investigators suggested a "survivor-cohort effect" that some of these patients might not have PCI performed in earlier years when primary PCI therapy was less prevalent. They further suggested that the expected increased mortality from this highrisk subset had offset the "gains" from shorter door-to-balloon times explaining why overall mortality had not fallen in later years [2].This explanation however did not ensure that primary PCI performed in more recent years was better than PCI in earlier years. There is another more pertinent interpretation for the "worsening" mortality -recent mainstream research has not targeted the critical "link" between STEMI management and STEMI outcome -i.e., reducing the total time duration between STEMI onset and successful myocardial reperfusion of which door-to-balloon time only constitutes a (small) portion.As shown in both studies [1,2] on the Cath-PCI registry over 2005 to 2011 there was an increasing use of thrombectomy (from ~10% tõ 40%) and direct thrombin inhibitor bivalirudin (from ~10% to ~40%) and a decreasing use of glycoprotein 2B3A inhibit...

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Measuring Platelet Reactivity after Clopidogrel-Has it Reached the End of the Road?

Cited by 6 publications

References 17 publications

Trials Evaluating Ticagrelor in Cardiovascular Disease: Will It Reign Supreme in the Anti-Platelet World?

Trials Evaluating Ticagrelor in Cardiovascular Disease: Will It Reign Supreme in the Anti-Platelet World?

From Arctic to Antarctic: Is There any Remaining Role for Platelet Function Testing to Tailor Therapy after Coronary Stent Implantation?

Time for a Reappraisal: How much has the Last 10 Years of Ã¢ÂÂMainstreamÃ¢ÂÂ STEMI Research Impacted on STEMI Outcome?

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Measuring Platelet Reactivity after Clopidogrel-Has it Reached the End of the Road?

Cited by 6 publications

References 17 publications

Trials Evaluating Ticagrelor in Cardiovascular Disease: Will It Reign Supreme in the Anti-Platelet World?

Trials Evaluating Ticagrelor in Cardiovascular Disease: Will It Reign Supreme in the Anti-Platelet World?

From Arctic to Antarctic: Is There any Remaining Role for Platelet Function Testing to Tailor Therapy after Coronary Stent Implantation?

Time for a Reappraisal: How much has the Last 10 Years of Ã¢ÂÂMainstreamÃ¢ÂÂ STEMI Research Impacted on STEMI Outcome?

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Time for a Reappraisal: How much has the Last 10 Years of Ã¢ÂÂMainstreamÃ¢ÂÂ STEMI Research Impacted on STEMI Outcome?