加拿大魁北克家族性高胆固醇血症的基因检测:一项单中心回顾性队列研究

CMAJ open Pub Date : 2023-07-01 DOI:10.9778/cmajo.20220108
Amanda Guerin, Iulia Iatan, Isabelle Ruel, Linda Fri Ngufor, Jacques Genest
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引用次数: 0

摘要

背景:家族性高胆固醇血症(FH)与低密度脂蛋白胆固醇(LDL-C)水平升高引起的过早动脉粥样硬化性心血管疾病相关。我们确定了完整的下一代测序(NGS)基因小组对魁北克临床诊断为FH的患者重新分类的影响,与魁北克卫生和社会服务部(MSSS)目前提供的部分基因小组进行比较,其中包括11种在法裔加拿大人中常见的变异。方法:我们在2017年9月至2021年9月期间,在montracimal的麦吉尔大学健康中心预防心脏病学/脂质诊所的加拿大FH登记处进行了一项回顾性队列研究,这些患者被临床诊断为严重高胆固醇血症,可能是FH或根据加拿大FH的定义确定为FH。对LDLR、APOB和PCSK9基因进行新一代测序,并对LDLR基因进行多重连接依赖探针扩增以检测遗传变异。结果:在连续335例杂合子FH患者中(男性184例[54.9%],女性151例[45.1%]),基线LDL-C水平为6.96(标准差1.79)mmol/L。通过级联筛查确定的患者比指数患者平均年轻11岁,并且有心血管危险因素的比例较小。229例接受基因检测的患者中有169例(73.8%)发现致病性FH变异;大多数患者存在LDLR(146例[86.4%])或APOB(24例[14.2%])基因变异。由MSSS提供的遗传面板仅占完整NGS面板识别的变异的48%。229例患者中,90例(39.3%,95%可信区间32.9%-46.0%)在FH全组基因筛查后从临床诊断的可能FH重新分类为明确FH。解释:对疑似患有FH的患者进行基因检测提供了诊断的确定性,并允许许多临床诊断为可能患有FH的患者被重新分类为患有明确的FH。基因筛查可以增加FH患者的识别,因此可能有助于减少加拿大FH患者的心血管疾病负担和死亡率。试验注册:ClinicalTrials.gov,编号:NCT02009345。
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Genetic testing for familial hypercholesterolemia in Quebec, Canada: a single-centre retrospective cohort study.

Background: Familial hypercholesterolemia (FH) is associated with premature atherosclerotic cardiovascular disease caused by elevated low-density lipoprotein cholesterol (LDL-C) levels. We determined the impact of a full next-generation sequencing (NGS) genetic panel on reclassification of patients with a clinical diagnosis of FH in Quebec compared to the partial genetic panel currently offered by the Quebec Ministère de la Santé et des Services sociaux (Ministry of Health and Social Services) (MSSS), which includes 11 variants that are common in French Canadians.

Methods: We conducted a retrospective cohort study in a subgroup of patients in the Canadian FH Registry seen at the McGill University Health Centre Preventive Cardiology/Lipid Clinic, Montréal, between September 2017 and September 2021 who were clinically diagnosed with severe hypercholesterolemia, probable FH or definite FH according to the Canadian definition of FH. Next-generation sequencing of the LDLR, APOB and PCSK9 genes, and multiplex ligation-dependent probe amplification of the LDLR gene to detect genetic variants, were performed.

Results: Among 335 consecutive patients with heterozygous FH (184 men [54.9%] and 151 women [45.1%]), the baseline LDL-C level was 6.96 (standard deviation 1.79) mmol/L. Patients identified through cascade screening were 11 years younger on average than index patients, and smaller proportions presented to the clinic with cardiovascular risk factors. A pathogenic FH variant was identified in 169 (73.8%) of the 229 patients who underwent genetic testing; the majority had variants in the LDLR (146 [86.4%]) or APOB (24 [14.2%]) gene. The genetic panel offered by the MSSS accounted for only 48% of the variants identified with the full NGS panel. Of the 229 patients, 90 (39.3%, 95% confidence interval 32.9%-46.0%) were reclassified from a clinical diagnosis of probable FH to definite FH after genetic screening with a full FH panel.

Interpretation: Genetic testing in patients suspected of having FH provided diagnostic certainty and permitted many patients with a clinical diagnosis of probable FH to be reclassified as having definite FH. Genetic screening allows for increased identification of patients with FH and may therefore help reduce the burden of cardiovascular disease and mortality rates among Canadians with FH. Trial registration: ClinicalTrials.gov, no. NCT02009345.

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