LDL-C AND POLYGENIC RISK FOR CORONARY HEART DISEASE RISK ASSESSMENT

IF 5.9 Q1 CARDIAC & CARDIOVASCULAR SYSTEMS

American journal of preventive cardiology Pub Date : 2025-09-01 DOI:10.1016/j.ajpc.2025.101101

Jamal Rana MD, PhD , Meng Lu MS , Roberto Elosua MD, PhD , Martha Gulati MD, MSc , Nathan D. Wong PhD, MPH , Carlos Iribarren MD, MPH, PhD

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引用次数: 0

Abstract

Therapeutic Area

ASCVD/CVD Risk Assessment

Background

Elevated concentrations of LDL-cholesterol (LDL-C) are a major independent modifiable risk factor for coronary heart disease (CHD). However, the joint consideration of LDL-C and background polygenic risk in assessing risk remains unclear.

Methods

We utilized data from a subset of the Genetic Epidemiology Resource in Adult Health and Aging (GERA) Multi-Ethnic cohort (n=47,576) who were without diabetes and not taking cholesterol lowering medication at baseline in 2007-2008. We stratified the cohort into three groups of CHD genetic risk (low=quintile 1; intermediate=quintiles 2, 3 and 4; and high=quintile 5) using a 12-SNP Polygenic Risk Score (PRS) for CHD (CARDIO inCode-Score, GENinCode Plc). Incident CHD consisted of primary in-patient codes for angina pectoris, myocardial infarction, revascularization procedures or CHD death through 12/31/2022 (n=1,678); mean follow-up was 13.8 years. Age-adjusted CHD rates per 10,000 person-years were estimated using Poisson regression (accounting for death and health plan disenrollment) according to polygenic risk and LDL-C level. Hazard ratios and 95% confidence intervals for 1 standard deviation (SD) increment of LDL-C in each PRS group were obtain using Cox regression adjusting for 10 principal components of ancestry plus traditional risk factors. We tested for formal interaction LDL-C*PRS as continuous variables in the fully adjusted model.

Results

Mean ± SD age = 58.1 ± 10.3 years; 62% female; 18% non-European ancestry. There were nonstatistically significant associations between LDL-C and incident CHD among low polygenic risk individuals, although individuals with severe hypercholesterolemia (≥190 mg/dL) in this group had a markedly elevated HR (2.3; p=0.06) (Table and forest plot). In the intermediate polygenic risk group, there was a steady increased risk of CHD as LDL-C increased, with markedly higher HR (>2.0) starting at 160 mg/dL. In the high polygenic risk group, HR of CHD began to increase markedly starting at LDL-C of 130 mg/dL, and the combination of both high polygenic risk and severe hypercholesterolemia (LDL-C > 190 mg/dL) was associated with a HR of 3.6.

Conclusions

These results have important clinical implications for lipid management in asymptomatic populations and support a more aggressive management and primary prevention for individuals with high polygenic risk.

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Ldl-c与冠心病多基因风险评估

背景低密度脂蛋白胆固醇（LDL-C）浓度降低是冠心病（CHD）的一个主要的独立可改变的危险因素。然而，在评估风险时是否联合考虑LDL-C和背景多基因风险仍不清楚。方法：我们利用了来自成人健康与老龄化遗传流行病学资源（GERA）多种族队列（n=47,576）的数据，这些人在2007-2008年没有糖尿病，也没有服用降胆固醇药物。我们使用冠心病的12个snp多基因风险评分（PRS）（CARDIO inCode-Score, GENinCode Plc）将队列分为三组冠心病遗传风险（低= 1分位数，中= 2、3和4分位数，高= 5分位数）。截至2022年12月31日，冠心病事件包括心绞痛、心肌梗死、血运重建术或冠心病死亡的主要住院患者代码（n=1,678）；平均随访时间为13.8年。根据多基因风险和LDL-C水平，使用泊松回归（考虑死亡和健康计划退出）估计每10,000人年的年龄调整冠心病发病率。采用Cox回归对10个主成分及传统危险因素进行校正，得到各PRS组LDL-C增加1个标准差（SD）的风险比和95%置信区间。在完全调整模型中，我们检验了LDL-C*PRS作为连续变量的形式相互作用。结果平均±SD年龄 = 58.1±10.3岁；62%的女性;18%是非欧洲血统。在低多基因风险个体中，LDL-C与冠心病发生率之间存在无统计学意义的关联，尽管该组中严重高胆固醇血症（≥190 mg/dL）个体的HR显著升高（2.3;p=0.06）（表和森林图）。在中等多基因风险组中，随着LDL-C的增加，冠心病的风险稳步增加，从160 mg/dL开始，HR （>2.0）显著升高。在高多基因风险组中，从LDL-C为130 mg/dL开始，冠心病的HR开始显著增加，高多基因风险和严重高胆固醇血症（LDL-C > 190 mg/dL）的合并与HR为3.6相关。结论这些结果对无症状人群的脂质管理具有重要的临床意义，并支持对高多基因风险个体进行更积极的管理和一级预防。

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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