Robyns Tomas, Kuiperi Cuno, Willems Rik, Corveleyn Anniek, Nuyens Dieter
Acta Cardiol. 2015 Dec;70(6):747-9. doi: 10.2143/AC.70.6.3120197.
We present a new mutation in KCNH2 (c.2038delG) resulting in a frameshift and premature truncation of the IKr channel protein in a large LQTS family with several sudden death cases. This mutation was initially missed by mutation scanning with DHPLC due to allelic dropout and only retrieved after repeat genetic testing with targeted capture and massive parallel sequencing. There was full penetrance of this mutation, only if an individualized QT correction derived from 24-hour Holter data was used. This case again underscores the importance of repeat genetic testing in robust cases of LQTS that remained genotype negative with mutation scanning techniques.
我们在一个有几例猝死病例的大型长QT综合征(LQTS)家系中发现了KCNH2基因的一个新突变(c.2038delG),该突变导致IKr通道蛋白发生移码和过早截断。由于等位基因缺失,该突变最初通过变性高效液相色谱(DHPLC)进行突变扫描时未被发现,仅在使用靶向捕获和大规模平行测序进行重复基因检测后才被检出。只有使用从24小时动态心电图数据得出的个体化QT校正值时,该突变才具有完全外显率。该病例再次强调了在LQTS确诊病例中进行重复基因检测的重要性,这些病例在用突变扫描技术检测时基因型仍为阴性。
