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致心肌病的致病性 DNA 变异与心血管疾病结局和全因死亡率的相关性研究。

Association of Pathogenic DNA Variants Predisposing to Cardiomyopathy With Cardiovascular Disease Outcomes and All-Cause Mortality.

机构信息

Division of Cardiology, Department of Medicine, Massachusetts General Hospital, Boston.

Center for Genomic Medicine, Department of Medicine, Massachusetts General Hospital, Boston.

出版信息

JAMA Cardiol. 2022 Jul 1;7(7):723-732. doi: 10.1001/jamacardio.2022.0901.

DOI:10.1001/jamacardio.2022.0901
PMID:35544052
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC9096692/
Abstract

IMPORTANCE

Pathogenic variants associated with inherited cardiomyopathy are recognized as important and clinically actionable when identified, leading some clinicians to recommend population-wide genomic screening.

OBJECTIVE

To determine the prevalence and clinical importance of pathogenic variants associated with inherited cardiomyopathy within the context of contemporary clinical care.

DESIGN, SETTING, AND PARTICIPANTS: This was a genetic association study of participants in Atherosclerosis in Risk Communities (ARIC), recruited from 1987 to 1989, with median follow-up of 27 years, and the UK Biobank, recruited from 2006 to 2010, with median follow-up of 10 years. ARIC participants were recruited from 4 sites across the US. UK Biobank participants were recruited from 22 sites across the UK. Participants in the US were of African and European ancestry; those in the UK were of African, East Asian, South Asian, and European ancestry. Statistical analyses were performed between August 1, 2021, and February 9, 2022.

EXPOSURES

Rare genetic variants predisposing to inherited cardiomyopathy.

MAIN OUTCOMES AND MEASURES

Pathogenicity of observed DNA sequence variants in sequenced exomes of 13 genes (ACTC1, FLNC, GLA, LMNA, MYBPC3, MYH7, MYL2, MYL3, PRKAG2, TNNI3, TNNT2, TPM1, and TTN) associated with inherited cardiomyopathies were classified by a blinded clinical geneticist per American College of Medical Genetics recommendations. Incidence of all-cause mortality, heart failure, and atrial fibrillation were determined. Cardiac magnetic resonance imaging, echocardiography, and electrocardiogram measures were assessed in a subset of participants.

RESULTS

A total of 9667 ARIC participants (mean [SD] age, 54.0 [5.7] years; 4232 women [43.8%]; 2658 African [27.5%] and 7009 European [72.5%] ancestry) and 49 744 UK Biobank participants (mean [SD] age, 57.1 [8.0] years; 27 142 women [54.5%]; 1006 African [2.0%], 173 East Asian [0.3%], 939 South Asian [1.9%], and 46 449 European [93.4%] European ancestry) were included in the study. Of those, 59 participants (0.61%) in ARIC and 364 participants (0.73%) in UK Biobank harbored an actionable pathogenic or likely pathogenic variant associated with dilated or hypertrophic cardiomyopathy. Carriers of these variants were not reliably identifiable by imaging. However, the presence of these variants was associated with increased risk of heart failure (hazard ratio [HR], 1.7; 95% CI, 1.1-2.8), atrial fibrillation (HR, 2.9; 95% CI, 1.9-4.5), and all-cause mortality (HR, 1.5; 95% CI, 1.1-2.2) in ARIC. Similar risk patterns were observed in the UK Biobank.

CONCLUSIONS AND RELEVANCE

Results of this genetic association study suggest that approximately 0.7% of study participants harbored a pathogenic variant associated with inherited cardiomyopathy. These variant carriers would be challenging to identify within clinical practice without genetic testing but are at increased risk for cardiovascular disease and all-cause mortality.

摘要

重要性

与遗传性心肌病相关的致病性变异被认为是重要的,并具有临床可操作性,当这些变异被识别出来时,一些临床医生建议进行人群范围的基因组筛查。

目的

在当代临床护理的背景下,确定与遗传性心肌病相关的致病性变异的患病率和临床重要性。

设计、地点和参与者:这是一项对 Atherosclerosis in Risk Communities (ARIC) 参与者的遗传关联研究,该研究于 1987 年至 1989 年招募,中位随访时间为 27 年,以及 UK Biobank,于 2006 年至 2010 年招募,中位随访时间为 10 年。ARIC 参与者来自美国的 4 个地点。UK Biobank 的参与者来自英国的 22 个地点。美国参与者的祖先是非洲裔和欧洲裔;英国参与者的祖先是非洲裔、东亚裔、南亚裔和欧洲裔。统计分析于 2021 年 8 月 1 日至 2022 年 2 月 9 日进行。

暴露情况

导致遗传性心肌病的罕见遗传变异。

主要结果和措施

通过美国医学遗传学学院的建议,由一位盲法临床遗传学家对 13 个与遗传性心肌病相关的基因(ACTC1、FLNC、GLA、LMNA、MYBPC3、MYH7、MYL2、MYL3、PRKAG2、TNNI3、TNNT2、TPM1 和 TTN)的测序外显子中观察到的 DNA 序列变异的致病性进行分类。确定全因死亡率、心力衰竭和心房颤动的发生率。在亚组参与者中评估了心脏磁共振成像、超声心动图和心电图测量结果。

结果

共有 9667 名 ARIC 参与者(平均[标准差]年龄 54.0[5.7]岁;4232 名女性[43.8%];2658 名非洲裔[27.5%]和 7009 名欧洲裔[72.5%])和 49744 名 UK Biobank 参与者(平均[标准差]年龄 57.1[8.0]岁;27142 名女性[54.5%];1006 名非洲裔[2.0%],173 名东亚裔[0.3%],939 名南亚裔[1.9%],46449 名欧洲裔[93.4%])被纳入研究。其中,59 名参与者(0.61%)在 ARIC 和 364 名参与者(0.73%)在 UK Biobank 中携带与扩张型或肥厚型心肌病相关的可操作的致病性或可能致病性变异。通过影像学无法可靠地识别这些变异的携带者。然而,这些变异的存在与心力衰竭(风险比[HR],1.7;95%CI,1.1-2.8)、心房颤动(HR,2.9;95%CI,1.9-4.5)和全因死亡率(HR,1.5;95%CI,1.1-2.2)的风险增加相关。在 UK Biobank 中也观察到了类似的风险模式。

结论和相关性

这项遗传关联研究的结果表明,大约 0.7%的研究参与者携带与遗传性心肌病相关的致病性变异。如果没有基因测试,在临床实践中很难识别这些变异携带者,但他们患心血管疾病和全因死亡率的风险增加。

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