Boczek Nicole J, Tester David J, Ackerman Michael J
Mayo Graduate School, Mayo Clinic, Rochester, MN, USA.
Herzschrittmacherther Elektrophysiol. 2012 Sep;23(3):167-73. doi: 10.1007/s00399-012-0222-x. Epub 2012 Sep 20.
Annually thousands of sudden deaths involving young individuals (<35 years of age) remain unexplained following a complete medicolegal investigation that includes an autopsy. In fact, epidemiological studies have estimated that over half of sudden deaths involving previously healthy young individuals have no morphological abnormalities identifiable at autopsy. Cardiac channelopathies associated with structurally normal hearts such as long QT syndrome (LQTS), catecholaminergic polymorphic ventricular tachycardia (CPVT), and Brugada syndrome (BrS), leave no evidence to be found at autopsy, leaving investigators to only speculate that a lethal arrhythmia might lie at the heart of a sudden unexplained death (SUD). In cases of autopsy-negative SUD, continued investigation, through the use of a cardiological and genetic evaluation of first- or second-degree relatives and/or a molecular autopsy, may pinpoint the underlying mechanism attributing to the sudden death and allow for the identification of living family members with the pathogenic substrate that renders them vulnerable to an increased risk for cardiac events, including sudden death.
每年,在包括尸检在内的完整法医学调查之后,仍有数千例涉及年轻人(<35岁)的猝死原因不明。事实上,流行病学研究估计,超过一半涉及此前健康年轻人的猝死在尸检时未发现形态学异常。与结构正常心脏相关的心脏离子通道病,如长QT综合征(LQTS)、儿茶酚胺能多形性室性心动过速(CPVT)和Brugada综合征(BrS),在尸检时找不到证据,使得调查人员只能推测致命性心律失常可能是不明原因猝死(SUD)的核心原因。在尸检阴性的SUD病例中,通过对一级或二级亲属进行心脏和基因评估及/或分子尸检继续进行调查,可能会查明导致猝死的潜在机制,并识别出携带致病基因的在世家庭成员,这些基因使他们易患包括猝死在内的心脏事件风险增加。
