Sudden arrhythmic death syndrome: familial evaluation identifies inheritable heart disease in the majority of families

医学 Brugada综合征 长QT综合征 心源性猝死 猝死 心脏病学 阿玛林 内科学 心脏病 心肌病 疾病 死因 肥厚性心肌病 儿科 心力衰竭 QT间期
作者
Elijah R. Behr,Chrysoula Dalageorgou,Michael Christiansen,Petros Syrris,Siân Hughes,Maite Tome,Edward Rowland,Steve Jeffery,William J. McKenna
出处
期刊:European Heart Journal [Oxford University Press]
卷期号:29 (13): 1670-1680 被引量:419
标识
DOI:10.1093/eurheartj/ehn219
摘要

At least 4% of sudden deaths are unexplained at autopsy [sudden arrhythmic death syndrome (SADS)] and a quarter may be due to inherited cardiac disease. We hypothesized that comprehensive clinical investigation of SADS families would identify more susceptible individuals and causes of death.Fifty seven consecutively referred families with SADS death underwent evaluation including resting 12 lead, 24 h and exercise ECG and 2D echocardiography. Other investigations included signal averaged ECG, ajmaline testing, cardiac magnetic resonance imaging, and mutation analysis. First-degree relatives [184/262 (70%)] underwent evaluation, 13 (7%) reporting unexplained syncope. Seventeen (30%) families had a history of additional unexplained premature sudden death(s). Thirty families (53%) were diagnosed with inheritable heart disease: 13 definite long QT syndrome (LQTS), three possible/probable LQTS, five Brugada syndrome, five arrhythmogenic right ventricular cardiomyopathy (ARVC), and four other cardiomyopathies. One SCN5A and four KCNH2 mutations (38%) were identified in 13 definite LQTS families, one SCN5A mutation (20%) in five Brugada syndrome families and one (25%) PKP2 (plakophyllin2) mutation in four ARVC families.Over half of SADS deaths were likely to be due to inherited heart disease; accurate identification is vital for appropriate prophylaxis amongst relatives who should undergo comprehensive cardiological evaluation, guided and confirmed by mutation analysis.
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