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Brugada Syndrome: Progress in Diagnosis and Management

机译:Brugada综合征:诊断和管理的进展

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摘要

Brugada syndrome (BrS) represents an inherited disorder associated with risk of sudden cardiac death due to VF in patients without structural heart disease. Currently, BrS is diagnosed by typical cove-shaped ST-segment elevation >2 mm in >1 RV precordial lead V1, V2 occurring spontaneously or after a sodium-channel blocker provocation test without any further evidence of malignant arrhythmias. An ICD should always be implanted in symptomatic BrS patients to prevent sudden death, despite high rates of complications with these devices. In asymptomatic people, an electrophysiological study should be performed to evaluate the need for an ICD. The recent discovery of a functional substrate has revolutionised our approach to the pathophysiology and management of BrS. Promising new therapeutic options have emerged in the last 3 years. Ajmaline is able to determine the extension of the substrate by prolonging the duration and fragmentation of abnormal epicardial electrograms. Substrate ablation results in the disappearance of both coved-type ECG and ventricular tachycardia/VF inducibility. These findings are clinically relevant, suggesting that epicardial ablation guided by ajmaline infusion may be an effective therapeutic option in BrS, potentially removing the need for ICD implantation.
机译:Brugada综合征(BrS)代表一种遗传性疾病,与无结构性心脏病的患者因VF导致心脏猝死有关。目前,BrS可通过自发或在钠通道阻滞剂激发试验后自然出现的> 1 RV胸前导联V1,V2中典型的凹形ST段抬高> 2 mm来诊断,而无任何进一步的恶性心律不齐的证据。尽管这些设备并发症发生率很高,但ICD应始终植入有症状的BrS患者中以防止猝死。在无症状的人群中,应进行电生理检查以评估是否需要ICD。功能性底物的最新发现彻底改变了我们对BrS的病理生理学和治疗方法。在过去的三年中出现了有希望的新治疗选择。 Ajmaline能够通过延长异常心外膜电图的持续时间和碎片来确定底物的扩展。基质消融导致凹型ECG和室性心动过速/ VF诱导性均消失。这些发现在临床上是相关的,提示以阿马琳输注指导的心外膜消融可能是BrS的有效治疗选择,可能消除了ICD植入的需要。

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