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Genotype‐Specific Risk Stratification and Management of Patients with Long QT Syndrome

机译:长QT综合征患者的基因型特定风险分层和管理

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摘要

Long QT syndrome (LQTS) is an inherited disorder associated with life‐threatening ventricular arrhythmias. An understanding of the relationship between the genotype and phenotype characteristics of LQTS can lead to improved risk stratification and management of this hereditary arrhythmogenic disorder. Risk stratification in LQTS relies on combined assessment of clinical, electrocardiographic, and mutations‐specific factors. Studies have shown that there are genotype‐specific risk factors for arrhythmic events including age, gender, resting heart rate, QT corrected for heart rate, prior syncope, the postpartum period, menopause, mutation location, type of mutation, the biophysical function of the mutation, and response to beta‐blockers. Importantly, genotype‐specific therapeutic options have been suggested. Lifestyle changes are recommended according to the prevalent trigger for cardiac events. Beta‐blockers confer greater benefit among patients with LQT1 with the greatest benefit among those with cytoplasmic loops mutations; specific beta‐blocker agents may provide greater protection than other agents in specific LQTS genotypes. Potassium supplementation and sex hormone–based therapy may protect patients with LQT2. Sodium channel blockers such as mexiletine, flecainide, and ranolazine could be treatment options in LQT3.
机译:长QT综合征(LQTS)是与威胁生命的室性心律失常相关的遗传性疾病。对LQTS基因型和表型特征之间关系的理解可以导致这种遗传性心律失常性疾病的风险分层和管理得到改善。 LQTS中的风险分层取决于临床,心电图和突变特异性因素的综合评估。研究表明,存在心律失常事件的基因型特异性危险因素,包括年龄,性别,静息心率,经心率校正的QT,先前的晕厥,产后时期,更年期,突变位置,突变类型,生物的生理功能突变以及对β受体阻滞剂的反应。重要的是,已经提出了基因型特异性的治疗选择。建议根据心脏病事件的普遍触发因素改变生活方式。 β受体阻滞剂在LQT1患者中受益更大,而在胞质环突变患者中受益最大。特定的β-受体阻滞剂可能会比特定LQTS基因型的其他药物提供更大的保护。补充钾和性激素疗法可能会保护LQT2患者。钠通道阻滞剂如美西律,氟卡尼和雷诺嗪可能是LQT3的治疗选择。

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