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Cover of Dual Antiplatelet Therapy Following Percutaneous Coronary Intervention: Clinical and Economic Impact of Standard Versus Extended Duration — Project Protocol

Dual Antiplatelet Therapy Following Percutaneous Coronary Intervention: Clinical and Economic Impact of Standard Versus Extended Duration — Project Protocol

CADTH Optimal Use Report

Current guidelines recommend that patients be given dual antiplatelet therapy (DAPT; combination of a P2Y12 inhibitor [clopidogrel, prasugrel, or ticagrelor] with acetylsalicylic acid [ASA]) ranging from six months to 12 months following percutaneous coronary intervention (PCI) with stenting, with the aim of preventing stent thrombosis and major adverse cardiac and cerebrovascular events (MACCEs). However, debate is ongoing about the optimal duration of DAPT; importantly, patient characteristics may be an important factor in treatment duration decisions. In some settings, DAPT for even less than six months may be appropriate (e.g., patients with high risk of bleeding), while other patients may derive greater benefit from extended DAPT (e.g., patients with high risk of stent thrombosis and low risk of bleeding). Previous reviews have reported an increased risk of death among patients who received DAPT for more than 12 months following PCI with stenting, but whether this risk is common across all patient subgroups is unclear.

Previous systematic reviews (SRs) have attempted to determine the optimal duration of DAPT; however, there is a paucity of data on the impact of specific patient characteristics or type of P2Y12 inhibitor on the effect estimate. One SR reported that extending DAPT beyond 12 months reduced the risk of stent thrombosis in patients without, but not with, acute coronary syndrome (ACS); however, no significant differences were reported in the risk of cardiovascular (CV) death or myocardial infarction (MI). A recent network metaanalysis (NMA) found that among patients randomized to ticagrelor, prasugrel, or clopidogrel, the risk of major adverse cardiac events and MI were lower with both ticagrelor and prasugrel compared with clopidogrel. Shah et al. reported a reduced risk of all-cause and CV death among patients randomized to ticagrelor compared with clopidogrel; however, whether these results are consistent at all durations of DAPT is unknown.

To make appropriate decisions, clinicians require a transparent and comprehensive review of the evidence to evaluate the potential benefits and harms associated with extending DAPT beyond 12 months after stenting to potentially personalize therapy and reach best patient outcomes. Such information may also inform P2Y12 inhibitor reimbursement policies by insurers because such policies may be limited to 12 months, in particular in the public sector. In this study, we will evaluate the comparative clinical effectiveness of different DAPT durations by performing an SR to assess the benefits and harms associated with extending DAPT beyond 12 months following PCI with stenting. We will also investigate the effect of extended DAPT in clinically relevant patient subgroups, including age, history of MI, ACS at presentation, diabetes, and smoking status, and the impact of individual P2Y12 inhibitors. Of note, the patient subgroups were selected based on the clinical components of the DAPT Score combined with consideration of findings from a recent clinical review that found different effects between shorter and longer DAPT duration for some subgroups; the selected subgroups were chosen because statistically significant differences were observed in key clinical outcomes when extended DAPT was used. In addition, we will evaluate the comparative cost-effectiveness of different DAPT durations; results from the clinical review will be used to inform clinical input for the economic evaluation.

About the Series

CADTH Optimal Use Report
ISSN: 1927-0127
Funding: CADTH receives funding from Canada’s federal, provincial, and territorial governments, with the exception of Quebec.

Suggested citation:

Dual antiplatelet therapy following percutaneous coronary intervention: clinical and economic impact of standard versus extended duration — project protocol. Ottawa: CADTH; 2018 Feb.

Disclaimer: The information in this document is intended to help Canadian health care decision-makers, health care professionals, health systems leaders, and policy-makers make well-informed decisions and thereby improve the quality of health care services. While patients and others may access this document, the document is made available for informational purposes only and no representations or warranties are made with respect to its fitness for any particular purpose. The information in this document should not be used as a substitute for professional medical advice or as a substitute for the application of clinical judgment in respect of the care of a particular patient or other professional judgment in any decision-making process. The Canadian Agency for Drugs and Technologies in Health (CADTH) does not endorse any information, drugs, therapies, treatments, products, processes, or services.

While care has been taken to ensure that the information prepared by CADTH in this document is accurate, complete, and up-to-date as at the applicable date the material was first published by CADTH, CADTH does not make any guarantees to that effect. CADTH does not guarantee and is not responsible for the quality, currency, propriety, accuracy, or reasonableness of any statements, information, or conclusions contained in any third-party materials used in preparing this document. The views and opinions of third parties published in this document do not necessarily state or reflect those of CADTH.

CADTH is not responsible for any errors, omissions, injury, loss, or damage arising from or relating to the use (or misuse) of any information, statements, or conclusions contained in or implied by the contents of this document or any of the source materials.

This document may contain links to third-party websites. CADTH does not have control over the content of such sites. Use of third-party sites is governed by the third-party website owners’ own terms and conditions set out for such sites. CADTH does not make any guarantee with respect to any information contained on such third-party sites and CADTH is not responsible for any injury, loss, or damage suffered as a result of using such third-party sites. CADTH has no responsibility for the collection, use, and disclosure of personal information by third-party sites.

Subject to the aforementioned limitations, the views expressed herein are those of CADTH and do not necessarily represent the views of Canada’s federal, provincial, or territorial governments or any third party supplier of information.

This document is prepared and intended for use in the context of the Canadian health care system. The use of this document outside of Canada is done so at the user’s own risk.

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Copyright © 2018 Canadian Agency for Drugs and Technologies in Health.

The copyright and other intellectual property rights in this document are owned by CADTH and its licensors. These rights are protected by the Canadian Copyright Act and other national and international laws and agreements. Users are permitted to make copies of this document for non-commercial purposes only, provided it is not modified when reproduced and appropriate credit is given to CADTH and its licensors.

Except where otherwise noted, this work is distributed under the terms of a Creative Commons Attribution-NonCommercial-NoDerivatives 4.0 International licence (CC BY-NC-ND), a copy of which is available at http://creativecommons.org/licenses/by-nc-nd/4.0/

Bookshelf ID: NBK525821PMID: 30260612

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