Comparison of oral anticoagulants for stroke prevention in atrial fibrillation using the UK clinical practice research Datalink Aurum: A reference trial (ARISTOTLE) emulation study.

IF 15.8 1区 医学 Q1 Medicine
PLoS Medicine Pub Date : 2024-08-29 eCollection Date: 2024-08-01 DOI:10.1371/journal.pmed.1004377
Emma Maud Powell, Usha Gungabissoon, John Tazare, Liam Smeeth, Paris J Baptiste, Turki M Bin Hammad, Angel Y S Wong, Ian J Douglas, Kevin Wing
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引用次数: 0

Abstract

Background: Stroke prevention guidance for patients with atrial fibrillation (AF) uses evidence generated from randomised controlled trials (RCTs). However, applicability to patient groups excluded from trials remains unknown. Real-world patient data provide an opportunity to evaluate outcomes in a trial analogous population of direct oral anticoagulants (DOACs) users and in patients otherwise excluded from RCTs; however, there remains uncertainty on the validity of methods and suitability of the data. Successful reference trial emulation can support the generation of evidence around treatment effects in groups excluded or underrepresented in trials. We used linked United Kingdom primary care data to investigate whether we could emulate the pivotal ARISTOTLE trial (apixaban versus warfarin) and extend the analysis to investigate the impact of warfarin time in therapeutic range (TTR) on results.

Methods and findings: Patients with AF in the UK Clinical Practice Research Datalink (CPRD Aurum) prescribed apixaban or warfarin from 1 January 2013 to 31 July 2019 were selected. ARISTOTLE eligibility criteria were applied to this population and matched to the RCT apixaban arm on baseline characteristics creating a trial-analogous apixaban cohort; this was propensity-score matched to warfarin users in the CPRD Aurum. ARISTOTLE outcomes were assessed using Cox proportional hazards regression stratified by prior warfarin exposure status during 2.5 years of patient follow-up and results benchmarked against the trial results before treatment effectiveness was further evaluated based on (warfarin) TTR. The dataset comprised 8,734 apixaban users and propensity-score matched 8,734 warfarin users. Results [hazard ratio (95% confidence interval)] confirmed apixaban noninferiority for stroke or systemic embolism (SE) [CPRD 0.98 (0.82,1.19) versus trial 0.79 (0.66,0.95)] and death from any cause [CPRD 1.03 (0.93,1.14) versus trial 0.89 (0.80,0.998)] but did not indicate apixaban superiority. Absolute event rates for stroke/SE were similar for apixaban in CPRD Aurum and ARISTOTLE (1.27%/year), whereas a lower event rate was observed for warfarin (CPRD Aurum 1.29%/year, ARISTOTLE 1.60%/year). Analysis by TTR suggested similar effectiveness of apixaban compared with poorly controlled warfarin (TTR < 0.75) for stroke/SE [0.91 (0.73, 1.14)], all-cause death [0.94 (0.84, 1.06)], and superiority for major bleeding [0.74 (0.63, 0.86)]. However, when compared with well-controlled warfarin (TTR ≥ 0.75), apixaban was associated with an increased hazard for all-cause death [1.20 (1.04, 1.37)], and there was no significant benefit for major bleeding [1.08 (0.90, 1.30)]. The main limitation of the study's methodology are the risk of residual confounding, channelling bias and attrition bias in the warfarin arm, and selection bias and misclassification in the analysis by TTR.

Conclusions: Analysis of noninterventional data generated results demonstrating noninferiority of apixaban versus warfarin consistent with prespecified benchmarking criteria. Unlike in ARISTOTLE, superiority of apixaban versus warfarin was not seen, possible due to the lower proportion of Asian patients and higher proportion of patients with well-controlled warfarin compared to ARISTOTLE. This methodological template can be used to investigate treatment effects of oral anticoagulants in patient groups excluded from or underrepresented in trials and provides a framework that can be adapted to investigate treatment effects for other conditions.

使用英国临床实践研究数据链 Aurum 对心房颤动患者预防中风的口服抗凝剂进行比较:参考试验 (ARISTOTLE) 模拟研究。
背景:针对心房颤动(房颤)患者的卒中预防指南采用了随机对照试验(RCT)中获得的证据。然而,对试验排除在外的患者群体的适用性仍是未知数。真实世界的患者数据为评估直接口服抗凝药(DOACs)使用者的类似试验人群以及被排除在随机对照试验之外的患者的疗效提供了机会;但是,方法的有效性和数据的适用性仍存在不确定性。成功的参照试验仿真可为被排除在试验之外或在试验中代表性不足的群体提供有关治疗效果的证据。我们利用链接的英国初级保健数据来研究我们是否可以仿效关键的ARISTOTLE试验(阿哌沙班与华法林),并扩展分析以研究华法林在治疗范围内的时间(TTR)对结果的影响:选取2013年1月1日至2019年7月31日期间英国临床实践研究数据链(CPRD Aurum)中开具阿哌沙班或华法林处方的房颤患者。将ARISTOTLE资格标准应用于这一人群,并根据基线特征与RCT阿哌沙班治疗组进行匹配,建立一个与试验类似的阿哌沙班队列;这一队列与CPRD Aurum中的华法林用户进行倾向分数匹配。在对患者进行 2.5 年的随访期间,使用 Cox 比例危险度回归对 ARISTOTLE 结果进行评估,并根据之前的华法林暴露状态对结果进行分层,然后根据(华法林)TTR 进一步评估治疗效果。数据集包括 8734 名阿哌沙班使用者和倾向分数匹配的 8734 名华法林使用者。结果[危险比(95% 置信区间)]证实阿哌沙班在中风或全身性栓塞(SE)[CPRD 0.98(0.82,1.19)与试验 0.79(0.66,0.95)]和任何原因导致的死亡[CPRD 1.03(0.93,1.14)与试验 0.89(0.80,0.998)]方面无劣效性,但并未表明阿哌沙班具有优越性。在 CPRD Aurum 和 ARISTOTLE 试验中,阿哌沙班的卒中/SE 绝对事件发生率相似(1.27%/年),而华法林的事件发生率较低(CPRD Aurum 1.29%/年,ARISTOTLE 1.60%/年)。按TTR分析表明,与控制不佳的华法林相比(TTR<0.75),阿哌沙班在卒中/SE[0.91 (0.73, 1.14)]、全因死亡[0.94 (0.84, 1.06)]和大出血[0.74 (0.63, 0.86)]方面具有相似的有效性。然而,与控制良好的华法林(TTR ≥ 0.75)相比,阿哌沙班与全因死亡[1.20 (1.04, 1.37)]的危险增加相关,且对大出血[1.08 (0.90, 1.30)]无明显益处。该研究方法的主要局限性在于华法林治疗组存在残余混杂因素、渠道偏倚和自然减员偏倚的风险,而TTR分析存在选择偏倚和分类错误的风险:对非介入数据的分析结果表明,阿哌沙班与华法林相比不存在劣效性,符合预先设定的基准标准。与ARISTOTLE不同的是,阿哌沙班与华法林相比没有发现优越性,这可能是由于与ARISTOTLE相比,亚洲患者比例较低,华法林控制良好的患者比例较高。这一方法模板可用于研究被排除在试验之外或在试验中代表性不足的患者群体的口服抗凝剂治疗效果,并提供了一个可用于研究其他疾病治疗效果的框架。
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来源期刊
PLoS Medicine
PLoS Medicine MEDICINE, GENERAL & INTERNAL-
CiteScore
17.60
自引率
0.60%
发文量
227
审稿时长
4-8 weeks
期刊介绍: PLOS Medicine is a prominent platform for discussing and researching global health challenges. The journal covers a wide range of topics, including biomedical, environmental, social, and political factors affecting health. It prioritizes articles that contribute to clinical practice, health policy, or a better understanding of pathophysiology, ultimately aiming to improve health outcomes across different settings. The journal is unwavering in its commitment to uphold the highest ethical standards in medical publishing. This includes actively managing and disclosing any conflicts of interest related to reporting, reviewing, and publishing. PLOS Medicine promotes transparency in the entire review and publication process. The journal also encourages data sharing and encourages the reuse of published work. Additionally, authors retain copyright for their work, and the publication is made accessible through Open Access with no restrictions on availability and dissemination. PLOS Medicine takes measures to avoid conflicts of interest associated with advertising drugs and medical devices or engaging in the exclusive sale of reprints.
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