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NCT00827411 Clinical Trial

Double Randomization of a Monitoring Adjusted Antiplatelet Treatment Versus a Common Antiplatelet Treatment for DES Implantation, and Interruption Versus Continuation of Double Antiplatelet Therapy

Coronary Artery Disease Clinical Trial

ARCTIC

Official title:
Double Randomization of a Monitoring Adjusted Antiplatelet Treatment Versus a Common Antiplatelet Treatment for DES Implantation, and a Interruption Versus Continuation of Double Antiplatelet Therapy, One Year After Stenting

Clinical Trial Details — Status: Completed

Administrative data
NCT number NCT00827411
Other study ID # P080403
Secondary ID
Status Completed
Phase Phase 4
First received January 13, 2009
Last updated April 11, 2013
Start date January 2009
Est. completion date January 2013

Study information
Verified date April 2013
Source Assistance Publique - Hôpitaux de Paris
Contact n/a
Is FDA regulated No
Health authority France: Ministry of Health
Study type Interventional

Clinical Trial Summary

Our first hypothesis is that dose adjustment of aspirin and clopidogrel based on biological monitoring reduces the rate of severe cardiovascular complications compared to a conventional strategy in patients scheduled for drug eluting stent implantation and followed up for one year. Our second hypothesis is that interruption of clopidogrel / Prasugrel after one year of a combined therapy of clopidogrel/Prasugrel and aspirin is associated with a higher rate of severe cardiovascular complications as compared with patients in whom aspirin and clopidogrel / Prasugrel is maintained during the subsequent 6 months of follow-up.

Description:

Participating Centers : 38 french high PCI volume (>700) centers Rationale: Clopidogrel / Prasugrel (75 mg/day), in combination with aspirin (75 mg/day), is currently the antiplatelet treatment of choice for prevention of stent thrombosis, and clinical trials have shown that, in high-risk patients, prolonged dual antiplatelet treatment is more effective than aspirin alone in preventing major cardiovascular events. However, despite the use of clopidogrel, a considerable number of patients continue to have cardiovascular events. Numerous in VITRO studies have shown that individual responsiveness to clopidogrel but also to aspirin is not uniform in all patients and is subject to inter- and intraindividual variability. The recent possibility of bedside monitoring of oral antiplatelet therapy offers the unique opportunity of tailoring antiplatelet therapy. However, the relevance of such strategy has never been evaluated in a randomized prospective adequately powered study having long term follow-up (rationale 1). Late state stent thrombosis, especially in the era of drug eluting stent and after interruption of OAT, is another important safety issue raising the questions of the modalities of interruption of dual OAT after one year according to the most recent updated recommendations. Can we switch from dual to single OAT after one year? If so, what is the ischemic hazard? (Rational 2) Our first hypothesis is that a strategy of dose adjustment of OAT based on biological monitoring reduces the rate of the combined ischemic endpoints of death, urgent revascularization, stent thrombosis and stroke as compared to a conventional strategy (local practice without monitoring) in patients scheduled for DES implantation and followed up for one year. Our second hypothesis is that interruption of clopidogrel after one year of dual OAT is associated with a higher rate of the same combined ischemic endpoints as compared with patients in whom dual OAT is maintained during the subsequent 6 months of follow-up. Objectives: 1) To demonstrate the superiority of the strategy of monitoring with dose adjustment in suboptimal responders (Monitoring Arm) as compared to a more conventional strategy (Conventional Arm) with fixed dose regimen of both oral antiplatelet agents in all patients as defined by the international guidelines to reduce the primary endpoint evaluated one year after DES implantation. 2) to demonstrate the superiority of a strategy of pursuit of a dual OAT beyond one year (Pursuit Arm) as compared to a strategy of interruption (Interruption Arm).

Duration of the participation : from 18 up to 30 months according to the time delay from study start to randomization. No participants will be excluded from the study at the exception of consent withdrawal. However, participants who have not been randomized for interruption or continuation of DAPT at the 12 month follow up visit will terminate the study

Number of patients: 2500 patients. This number was obtained for the demonstration of the superiority of the strategy of monitoring (Monitoring Arm) over the conventional strategy (Conventional Arm) to reduce the primary endpoint by 33% (relative risk reduction).

Expected results: The ARCTIC study will provide answers to two major clinical challenges. It will also give a unique opportunity to assess the prevalence and the associated risk factors of suboptimal answers to OAT, but also to improve a suboptimal biological response. Finally, the economic impact of both strategies of monitoring and of interruption will be evaluated.

Recruitment information / eligibility
Status Completed
Enrollment 2500
Est. completion date January 2013
Est. primary completion date March 2012
Accepts healthy volunteers No
Gender Both
Age group 18 Years and older
Eligibility Inclusion Criteria:

- Patients (=18 years) in whom elective DES stent placement is scheduled after diagnostic angiography

- Patients not treated by GPIIb/IIIa inhibitors prior to randomization.

- Provided written consent for participation in the trial prior to any study-specific procedures or requirements.

Exclusion Criteria:

- Oral anticoagulation (Vitamin K Antagonists).

- Contraindication for aspirin and/or clopidogrel/Prasugrel or GPIIb/IIIa inhibitors or to increasing dose of clopidogrel or aspirin

- Ongoing or recent bleeding and/or recent major surgery (<3 weeks)

- Severe liver dysfunction

- Thrombocytopenia (Platelet count <80000/µl).

- IIb/IIIa inhibitors within a week prior to randomization

- STEMI presentation

- Patient at risk of poor compliance to the study

- Patient not affiliated to social security

- Pregnant women, no signed inform consent

- Any invasive or surgical planned intervention during the year after stent placement

Study Design

Allocation: Randomized, Endpoint Classification: Efficacy Study, Intervention Model: Parallel Assignment, Masking: Open Label, Primary Purpose: Treatment

Related Conditions & MeSH terms

Intervention

Drug:
Aspirin and clopidogrel / Prasugrel
modification of aspirin and clopidogrel/Prasugrel maintenance doses based on a biological assay
Device:
VerifyNow
point of care assay VerifyNow (ACCUMETRICS San Diego USA)
Drug:
Aspirin and clopidogrel / Prasugrel
aspirin and clopidogrel/ Prasugrel maintenance doses (according to international guidelines)
Aspirin and clopidogrel / Prasugrel
maintenance dose of clopidogrel / Prasugrel and aspirin
Aspirin
Interruption of clopidogrel / Prasugrel after one year of follow-up

Locations
Country Name City State
France Institut de Cardiologie- Hopital la Pitié Salpétrière Paris

Sponsors (10)
Lead Sponsor Collaborator
Assistance Publique - Hôpitaux de Paris Allies in Cardiovascular Trials Initiatives and Organized, Boston Scientific Corporation, Bristol-Myers Squibb, Cordis Corporation, Diagnostica Stago, Fondation de France, Institut National de la Santé Et de la Recherche Médicale, France, Medtronic, Sanofi

Country where clinical trial is conducted

France, 

References & Publications (2)

Collet JP, Cayla G, Cuisset T, Elhadad S, Rangé G, Vicaut E, Montalescot G. Randomized comparison of platelet function monitoring to adjust antiplatelet therapy versus standard of care: rationale and design of the assessment with a double randomization of — View Citation

Collet JP, Cuisset T, Rangé G, Cayla G, Elhadad S, Pouillot C, Henry P, Motreff P, Carrié D, Boueri Z, Belle L, Van Belle E, Rousseau H, Aubry P, Monségu J, Sabouret P, O'Connor SA, Abtan J, Kerneis M, Saint-Etienne C, Barthélémy O, Beygui F, Silvain J, V — View Citation

Outcome
Type Measure Description Time frame Safety issue
Primary Composite endpoint of death, myocardial infarction, stroke, urgent coronary revascularization, stent thrombosis assessed at one year for the first hypothesis and between 6 up to 18 months of follow-up for the second hypothesis during the study (one year in both " monitoring " and " conventional " arms and during the periode from 6 up to 18 months in the "interruption" and "pursuit" arms) No
Secondary Stent thrombosis and urgent coronary revascularization at month 12 for the non-randomized patients at M12
at month 12 and month 30 for the randomized patient		 at month 12 and month 30 No
Secondary Rate of individual event at one year follow-up in both " monitoring " and " conventional " arms but also during the period from one year up to 24 months in the " interruption " and " pursuit " arms. at month 12 for the non-randomized patients at M12
at month 12 and month 30 for the randomized patient		 at month 12 and month 30 No
Secondary Time delay from treatment interruption (randomization 2) to any thrombotic event (stent thrombosis, urgent revascularization, acute myocardial infarction, cardiac death) treatment interruption(randomisation 2) at month 12 for the non-randomized patients at M12
at month 12 and month 30 for the randomized patient		 at month 12 and month 30 No
Secondary Treatment compliance evaluated by the number of oral antiplatelet treatment in both arms and with respect to all individual events of the primary composite endpoint at month 12 for the non-randomized patients at M12
at month 12 and month 30 for the randomized patient		 at month 12 and month 30 No
Secondary Rate of use of GP IIb/IIIa receptor antagonists in both " monitoring " and " conventional " arms before percutaneous coronary intervention and in bail out situations and in both. at month 12 for the non-randomized patients at M12
at month 12 and month 30 for the randomized patient		 at month 12 and month 30 No
Secondary Rate of suboptimal responders as defined by ARU>550 for aspirin or by a % of inhibition <15% and or a PRU<235) and the average dosage of aspirin and clopidogrel (in mg) will evaluated before and after dose adjustment (J0) and after each dose adjustment at month 12 for the non-randomized patients at M12
at month 12 and month 30 for the randomized patient		 at month 12 and month 30 No
Secondary Net clinical benefit (death, myocardial infarction, urgent revascularization, stent thrombosis, stroke, major bleeding) at month 12 for the non-randomized patients at M12
at month 12 and month 30 for the randomized patient		 at month 12 and month 30 No
Secondary Medico-economic evaluations will be performed for both hypotheses. The rate of rehospitalisation and the length of stay will be used as economic indicators at month 12 for the non-randomized patients at M12
at month 12 and month 30 for the randomized patient		 at month 12 and month 30 No
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