Department of Epidemiology, Biostatistics, and Occupational Health (H.W., S.Z., S.R.B., J.B.R.), Lady Davis Institute, Jewish General Hospital, Montréal, QC, Canada.
Center for Clinical Epidemiology (H.W., V.F., S.Z., J.B.R.), Lady Davis Institute, Jewish General Hospital, Montréal, QC, Canada.
Circ Genom Precis Med. 2021 Feb;14(1):e003106. doi: 10.1161/CIRCGEN.120.003106. Epub 2021 Jan 13.
The clinical implications of a polygenic risk score (PRS) for LDL-C (low-density lipoprotein cholesterol) are not well understood, both within the general population and individuals with familial hypercholesterolemia (FH).
We developed the LDL-C PRS using Least Absolute Shrinkage and Selection Operator regression in 377 286 White British participants from UK Biobank and tested its association with LDL-C according to FH variant carrier status in another 41 748 whole-exome sequenced individuals. Next, we tested for an enrichment of FH variant carriers among individuals with severe hypercholesterolemia and low LDL-C PRS. Last, we contrasted the effect of the LDL-C PRS, measured LDL-C and FH variant carrier status on risk of ischemic heart disease among 3010 cases and 38 738 controls.
Among the 41 748 whole-exome sequenced White British individuals, 1-SD increase in the LDL-C PRS was associated with elevated LDL-C among both FH variant carriers (0.34 [95% CI, 0.22-0.47] mmol/L) and noncarriers (0.42 [95% CI, 0.42-0.43] mmol/L). Among individuals with severe hypercholesterolemia, FH variant carriers were enriched in those with a low LDL-C PRS (odds ratio, 2.20 [95% CI, 1.66-2.71] per SD). Each SD increase in the LDL-C PRS was associated with risk of ischemic heart disease to the comparable magnitude as measured LDL-C (odds ratio, 1.24 [95% CI, 1.20-1.29] and odds ratio, 1.15 [95% CI, 1.09-1.23], respectively). The LDL-C PRS was not strongly associated with other traditional ischemic heart disease risk factors.
An LDL-C PRS could be used to identify individuals with a higher probability of harboring FH variants. The association between ischemic heart disease and the LDL-C PRS was comparable to measured LDL-C, likely because the PRS reflects lifetime exposure to LDL-C levels.
低密度脂蛋白胆固醇(LDL-C)多基因风险评分(PRS)在普通人群和家族性高胆固醇血症(FH)患者中的临床意义尚不清楚。
我们使用英国生物库中 377286 名白种英国人的数据,采用最小绝对收缩和选择算子回归法(Least Absolute Shrinkage and Selection Operator regression)开发了 LDL-C PRS,并在另外 41748 名全外显子组测序个体中根据 FH 变异携带者状态检验了其与 LDL-C 的相关性。接下来,我们检验了严重高胆固醇血症患者中,LDL-C PRS 低值患者 FH 变异携带者的富集情况。最后,我们比较了 LDL-C PRS、测定的 LDL-C 和 FH 变异携带者状态在 3010 例病例和 38738 例对照者中对缺血性心脏病风险的影响。
在 41748 名白种英国人全外显子组测序个体中,LDL-C PRS 每增加 1 个标准差(SD),FH 变异携带者(0.34[95%置信区间,0.22-0.47]mmol/L)和非携带者(0.42[95%置信区间,0.42-0.43]mmol/L)的 LDL-C 水平均升高。在严重高胆固醇血症患者中,FH 变异携带者在 LDL-C PRS 值较低的患者中更为富集(优势比,每 SD 增加 2.20[95%置信区间,1.66-2.71])。LDL-C PRS 每增加 1 个 SD,与缺血性心脏病的风险相关程度与测定的 LDL-C 相当(比值比,1.24[95%置信区间,1.20-1.29]和比值比,1.15[95%置信区间,1.09-1.23])。LDL-C PRS 与其他传统的缺血性心脏病危险因素的相关性并不强。
LDL-C PRS 可用于识别更有可能携带 FH 变异的个体。缺血性心脏病与 LDL-C PRS 的相关性与测定的 LDL-C 相当,这可能是因为 PRS 反映了终生 LDL-C 水平的暴露情况。
