William Harvey Research Institute, Queen Mary University of London, United Kingdom.
Barts Heart Centre, St Bartholomew's Hospital, Barts Health NHS Trust, West Smithfield, London, United Kingdom.
JAMA Cardiol. 2024 Nov 1;9(11):964-972. doi: 10.1001/jamacardio.2024.2190.
The population prevalence of cardiac transthyretin amyloidosis (ATTR) caused by pathogenic variation in the TTR gene (vATTR) is unknown.
To estimate the population prevalence of disease-causing TTR variants and evaluate associated phenotypes and outcomes.
DESIGN, SETTING, AND PARTICIPANTS: This population-based cohort study analyzed UK Biobank (UKB) participants with whole-exome sequencing, electrocardiogram, and cardiovascular magnetic resonance data. Participants were enrolled from 2006 to 2010, with a median follow-up of 12 (IQR, 11-13) years (cutoff date for the analysis, March 12, 2024). Sixty-two candidate TTR variants were extracted based on rarity (minor allele frequency ≤0.0001) and/or previously described associations with amyloidosis if more frequent.
Carrier status for TTR variants.
Associations of TTR carrier status with vATTR prevalence and cardiovascular imaging and electrocardiogram traits were explored using descriptive statistics. Associations between TTR carrier status and atrial fibrillation, conduction disease, heart failure, and all-cause mortality were evaluated using adjusted Cox proportional hazards models. Genotypic and diagnostic concordance was examined using International Statistical Classification of Diseases, Tenth Revision codes from the hospital record.
The overall cohort included 469 789 UKB participants (mean [SD] age, 56.5 [8.1] years; 54.2% female and 45.8% male). A likely pathogenic/pathogenic (LP/P) TTR variant was detected in 473 (0.1%) participants, with Val142Ile being the most prevalent (367 [77.6%]); 91 individuals (0.02%) were carriers of a variant of unknown significance . The overall prevalence of LP/P variants was 0.02% (105 of 444 243) in participants with European ancestry and 4.3% (321 of 7533) in participants with African ancestry. The LP/P variants were associated with higher left ventricular mass indexed to body surface area (β = 4.66; 95% CI, 1.87-7.44), and Val142Ile was associated with a longer PR interval (β = 18.34; 95% CI, 5.41-31.27). The LP/P carrier status was associated with a higher risk of heart failure (hazard ratio [HR], 2.68; 95% CI, 1.75-4.12) and conduction disease (HR, 1.88; 95% CI, 1.25-2.83). Higher all-cause mortality risk was observed for non-Val142Ile LP/P variants (HR, 1.98; 95% CI, 1.06-3.67). Thirteen participants (2.8%) with LP/P variants had diagnostic codes compatible with cardiac or neurologic amyloidosis. Variants of unknown significance were not associated with outcomes.
This study found that approximately 1 in 1000 UKB participants were LP/P TTR variant carriers, exceeding previously reported prevalence. The findings emphasize the need for clinical vigilance in identifying individuals at risk of developing vATTR and associated poor outcomes.
由 TTR 基因(vATTR)致病性变异引起的心脏转甲状腺素蛋白淀粉样变性(ATTR)的人群患病率尚不清楚。
评估致病 TTR 变异的人群患病率,并评估相关表型和结局。
设计、地点和参与者:本基于人群的队列研究分析了英国生物库(UKB)参与者的全外显子组测序、心电图和心血管磁共振数据。参与者于 2006 年至 2010 年期间入组,中位随访时间为 12(IQR,11-13)年(分析截止日期为 2024 年 3 月 12 日)。根据罕见性(次要等位基因频率≤0.0001)和/或先前描述的与淀粉样变性的相关性,从 62 个候选 TTR 变异中提取了更频繁的变异。
TTR 变异携带者状态。
使用描述性统计方法探讨 TTR 携带者状态与 vATTR 患病率以及心血管成像和心电图特征的关系。使用调整后的 Cox 比例风险模型评估 TTR 携带者状态与心房颤动、传导疾病、心力衰竭和全因死亡率之间的关系。使用医院记录中的国际疾病分类第十次修订代码检查基因和诊断的一致性。
整个队列包括 469789 名 UKB 参与者(平均[标准差]年龄为 56.5[8.1]岁;54.2%为女性,45.8%为男性)。在 473 名(0.1%)参与者中检测到可能致病性/致病性(LP/P)TTR 变异,其中 Val142Ile 最常见(367[77.6%]);91 名(0.02%)参与者为未知意义变异的携带者。在欧洲血统的参与者中,LP/P 变体的总体患病率为 0.02%(105/444243),在非洲血统的参与者中为 4.3%(321/7533)。LP/P 变体与更高的左心室质量指数(β=4.66;95%CI,1.87-7.44)相关,Val142Ile 与更长的 PR 间隔相关(β=18.34;95%CI,5.41-31.27)。LP/P 携带者状态与心力衰竭(危险比[HR],2.68;95%CI,1.75-4.12)和传导疾病(HR,1.88;95%CI,1.25-2.83)的风险增加相关。非 Val142Ile LP/P 变体的全因死亡率风险更高(HR,1.98;95%CI,1.06-3.67)。13 名(2.8%)携带 LP/P 变体的参与者有符合心脏或神经淀粉样变性的诊断代码。未知意义的变异与结局无关。
本研究发现,大约每 1000 名 UKB 参与者中有 1 名是 LP/P TTR 变体携带者,超过了先前报告的患病率。这些发现强调了在识别有发生 vATTR 风险和相关不良结局风险的个体时需要进行临床监测。
