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使用多种心血管危险因素多基因风险评分预测心房和心室心律失常。

Prediction of atrial and ventricular arrhythmias using multiple cardiovascular risk-factor polygenic risk scores.

作者信息

Ramírez Julia, van Duijvenboden Stefan, Orini Michele, Lambiase Pier D, Tinker Andrew, Young William J, Munroe Patricia B

机构信息

Aragon Institute of Engineering Research, University of Zaragoza, Zaragoza, Spain; Centro de Investigación Biomédica en Red-Bioingeniería, Biomateriales y Nanomedicina, Spain; William Harvey Research Institute, Barts and the London Faculty of Medicine and Dentistry, Queen Mary University of London, London, UK.

William Harvey Research Institute, Barts and the London Faculty of Medicine and Dentistry, Queen Mary University of London, London, UK; Nuffield Department of Population Health, University of Oxford, Oxford, UK; Institute of Cardiovascular Science, University College London, London, UK.

出版信息

Heart Rhythm. 2025 Sep;22(9):2361-2371. doi: 10.1016/j.hrthm.2024.12.017. Epub 2024 Dec 15.

Abstract

BACKGROUND

Atrial fibrillation (AF) prediction improves by combining clinical scores with a polygenic risk score (PRS) for AF (AF-PRS), but there are limited studies of PRS for ventricular arrhythmia (VA) prediction.

OBJECTIVE

We assessed the value of including multiple PRS for cardiovascular risk factors (CV-PRS) for incident AF and VA prediction.

METHODS

We used 158,733 individuals of European ancestry from UK Biobank to build 3 models for AF: CHARGE-AF (AF1), AF1 + AF-PRS (AF2), AF2 + CV-PRS (AF3). Models for VA included sex and age (VA1), VA1 + coronary artery disease (CAD) PRS (CAD-PRS, VA2), and VA2 + CV-PRS (VA3), conducting separate analyses in subjects with and without ischemic heart disease (IHD). Performance was evaluated in individuals of European (N = 158,733), African (N = 7200), South Asian (N = 9241) and East Asian (N = 2076) ancestry from UK Biobank.

RESULTS

AF2 had a higher C-index than AF1 (0.762 vs 0.746, P < .001), marginally improving to 0.765 for AF3 (P < .001, including PRS for heart failure, electrocardiogram and cardiac magnetic resonance measures). In South Asians, AF2 C-index was higher than AF1 (P < .001). For VA, the C-index for VA2 was greater than VA1 (0.692 vs 0.681, P < .001) in Europeans, which was also observed in South Asians (P < .001). VA3 improved prediction of VA in individuals with IHD.

CONCLUSION

CV-PRS improved AF prediction compared to CHARGE-AF and AF-PRS. A CAD-PRS improved VA prediction, while CV-PRS contributed in IHD. AF- and CAD-PRS were transferable to individuals of South Asian ancestry. Our results inform of the use of CV-PRS for personalized screening.

摘要

背景

通过将临床评分与心房颤动(AF)的多基因风险评分(PRS)(AF-PRS)相结合,可改善AF预测,但关于用于室性心律失常(VA)预测的PRS的研究有限。

目的

我们评估纳入多种心血管危险因素的PRS(CV-PRS)对新发AF和VA预测的价值。

方法

我们使用英国生物银行中158733名欧洲血统个体构建了3种AF模型:CHARGE-AF(AF1)、AF1 + AF-PRS(AF2)、AF2 + CV-PRS(AF3)。VA模型包括性别和年龄(VA1)、VA1 + 冠状动脉疾病(CAD)PRS(CAD-PRS,VA2)以及VA2 + CV-PRS(VA3),在有和没有缺血性心脏病(IHD)的受试者中进行单独分析。在英国生物银行中欧洲(N = 158733)、非洲(N = 7200)、南亚(N = 9241)和东亚(N = 2076)血统的个体中评估性能。

结果

AF2的C指数高于AF1(0.762对0.746,P <.001),AF3略微提高到0.765(P <.001,包括心力衰竭、心电图和心脏磁共振测量的PRS)。在南亚人中,AF2的C指数高于AF1(P <.001)。对于VA,在欧洲人中,VA2的C指数大于VA1(0.692对0.681,P <.001),在南亚人中也观察到这种情况(P <.001)。VA3改善了IHD个体中VA的预测。

结论

与CHARGE-AF和AF-PRS相比,CV-PRS改善了AF预测。CAD-PRS改善了VA预测,而CV-PRS在IHD中起作用。AF-和CAD-PRS可转移到南亚血统个体。我们的结果为使用CV-PRS进行个性化筛查提供了依据。

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