Effect of disclosing a polygenic risk score for coronary heart disease on adverse cardiovascular events: 10-year follow-up of the MI-GENES randomized clinical trial

Mohammadreza Naderian, Marwan E. Hamed, Ali A. Vaseem, Kristjan Norland, Ozan Dikilitas, Azin Teymourzadeh, Kent R. Bailey, Iftikhar J. Kullo
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Abstract

Background: The MI-GENES clinical trial (NCT01936675), in which participants at intermediate risk of coronary heart disease (CHD) were randomized to receive a Framingham risk score (FRSg, n=103), or an integrated risk score (IRSg, n=104) that additionally included a polygenic risk score (PRS), demonstrated that after 6 months, participants randomized to IRSg had higher statin initiation and lower low-density lipoprotein cholesterol (LDL-C). Objectives: In a post hoc 10-year follow-up analysis of the MI-GENES trial, we investigated whether disclosure of a PRS for CHD was associated with a reduction in adverse cardiovascular events. Methods: Participants were followed from randomization beginning in October 2013 until September 2023 to ascertain adverse cardiovascular events, testing for CHD, and changes in risk factors, by blinded review of electronic health records. The primary outcome was the time from randomization to the occurrence of the first major adverse cardiovascular event (MACE), defined as cardiovascular death, non-fatal myocardial infarction, coronary revascularization, and non-fatal stroke. Statistical analyses were conducted using Cox proportional hazards regression and linear mixed-effects models. Results: We followed all 203 participants who completed the MI-GENES trial, 100 in FRSg and 103 in IRSg (mean age at the end of follow-up: 68.2+-5.2, 48% male). During a median follow-up of 9.5 years, 9 MACEs occurred in FRSg and 2 in IRSg (hazard ratio (HR), 0.20; 95% confidence interval (CI), 0.04 to 0.94; P=0.042). In FRSg, 47 (47%) underwent at least one test for CHD, compared to 30 (29%) in IRSg (HR, 0.51; 95% CI, 0.32 to 0.81; P=0.004). IRSg participants had a longer duration of statin therapy during the first four years post-randomization and a greater reduction in LDL-C for up to 3 years post-randomization. No significant differences between the two groups were observed for hemoglobin A1C, systolic and diastolic blood pressures, weight, and smoking cessation rate during follow-up. Conclusions: The disclosure of an IRS that included a PRS to individuals at intermediate risk for CHD was associated with a lower incidence of MACE after a decade of follow-up, likely due to a higher rate of initiation and longer duration of statin therapy, leading to lower LDL-C levels.
公开冠心病多基因风险评分对不良心血管事件的影响:MI-GENES随机临床试验的10年随访
研究背景MI-GENES临床试验(NCT01936675)显示,6个月后,随机接受IRSg的参与者开始服用他汀类药物的比例更高,低密度脂蛋白胆固醇(LDL-C)更低:在对 MI-GENES 试验进行的一项为期 10 年的事后跟踪分析中,我们研究了披露 CHD PRS 是否与不良心血管事件的减少有关。研究方法:通过对电子健康记录进行盲法审查,从 2013 年 10 月开始的随机化到 2023 年 9 月对参与者进行随访,以确定不良心血管事件、心脏病检测和风险因素的变化。主要结果是从随机化到发生首次主要心血管不良事件(MACE)的时间,MACE定义为心血管死亡、非致死性心肌梗死、冠状动脉血运重建和非致死性中风。统计分析采用 Cox 比例危险回归和线性混合效应模型:我们对完成 MI-GENES 试验的所有 203 名参与者进行了随访,其中 FRSg 100 人,IRSg 103 人(随访结束时的平均年龄为 68.2+-5.2 岁,48% 为男性)。在中位随访 9.5 年期间,FRSg 和 IRSg 分别发生了 9 起和 2 起 MACE(危险比 (HR),0.20;95% 置信区间 (CI),0.04 至 0.94;P=0.042)。在 FRSg 患者中,47 人(47%)至少接受了一次冠心病检测,而在 IRSg 患者中,30 人(29%)至少接受了一次冠心病检测(HR,0.51;95% CI,0.32 至 0.81;P=0.004)。IRSg参与者在随机后的前四年中接受他汀类药物治疗的时间更长,而在随机后的三年中,LDL-C的降幅更大。在随访期间,两组在血红蛋白 A1C、收缩压和舒张压、体重和戒烟率方面没有观察到明显差异:结论:向冠心病中危人群披露包括 PRS 的 IRS 与随访十年后 MACE 发生率较低有关,这可能是由于他汀类药物治疗的启动率较高且持续时间较长,从而降低了 LDL-C 水平。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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