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Meta-Analysis of Risk Stratification of SCN5A With Brugada Syndrome: Is SCN5A Always a Marker of Low Risk?

机译:患有Brugada综合征的SCN5A风险分层的荟萃分析:SCN5A始终是低风险的标志吗?

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Background: SCN5A with Brugada syndrome (BrS) is not commonly considered as an independent risk marker for subsequent cardiac events. However, the risk of SCN5A combined with other clinical characteristics has not been fully investigated. Objectives: The aim of this study is to investigate and evaluate risk stratification and related risk factors of SCN5A in BrS. Methods: The databases of PubMed, EMBASE, Cochrane Library, MEDLINE, Chinese National Knowledge Infrastructure (CNKI) and Wanfang Data were searched for related studies published from January 2002 to May 2018 followed by meta-analysis. The BrS patients who underwent SCN5A gene tests were included. The prognosis and risk stratification of SCN5A combined with symptoms and asymptoms diagnosis in BrS, electrophysiology study (EPS) were then investigated and evaluated. Outcomes were defined as ventricular tachycardia/fibrillation (VT/VF), sudden cardiac death (SCD). Results: Eleven suitable studies involving 1892 BrS patients who underwent SCN5A gene tests were identified. SCN5A (+) was not considered to be a significant predictor of future cardiac events (95% CI: 0.89–2.11; P = 0.15; I ~(2) = 0%). However, SCN5A (+) patients with symptoms at diagnosis revealed a higher prevalence of future VT/VF, SCD compared to SCN5A (–) patients with symptoms at diagnosis. (95% CI: 1.06–3.70; P = 0.03 I ~(2) = 0%) Among asymptomatic patients, the risk did not significantly differ between SCN5A (+) patients and SCN5A (–) patients. (95% CI: 0.51–4.72; P = 0.45 I ~(2) = 0 %). In an investigation involving patients in EPS (–) BrS electrocardiogram (ECG), the risk of SCN5A (+) is higher than that of SCN5A (–) ( P & 0.001). Conclusions: In BrS patients with symptoms at diagnosis or EPS (–), the meta-analysis suggests that SCN5A (+) are at a higher risk of arrhythmic events than SCN5A (–).
机译:背景:患有Brugada综合征(BrS)的SCN5A通常不被视为随后发生心脏事件的独立风险标志。但是,尚没有对SCN5A与其他临床特征相结合的风险进行全面研究。目的:本研究旨在调查和评估BrS中SCN5A的危险分层和相关危险因素。方法:检索2002年1月至2018年5月发表的PubMed,EMBASE,Cochrane图书馆,MEDLINE,中国国家知识基础设施(CNKI)和万方数据的数据库,然后进行荟萃分析。包括接受SCN5A基因检测的BrS患者。然后,对SCN5A的预后和危险分层,并结合BrS,电生理研究(EPS)中的症状和无症状诊断进行了评估。结果定义为室性心动过速/纤颤(VT / VF),心源性猝死(SCD)。结果:确定了11项合适的研究,这些研究涉及1892名接受SCN5A基因测试的BrS患者。 SCN5A(+)不被认为是未来心脏事件的重要预测指标(95%CI:0.89–2.11; P = 0.15; I〜(2)= 0%)。但是,与诊断时有症状的SCN5A(-)患者相比,诊断为SCN5A(+)的患者显示出未来VT / VF,SCD的患病率更高。 (95%CI:1.06-3.70; P = 0.03 I〜(2)= 0%)在无症状患者中,SCN5A(+)患者和SCN5A(–)患者的风险无显着差异。 (95%CI:0.51–4.72; P = 0.45 I〜(2)= 0%)。在一项涉及EPS(-)BrS心电图(ECG)患者的调查中,SCN5A(+)的风险高于SCN5A(-)的风险(P <0.001)。结论:在具有诊断或EPS症状的BrS患者中(-),荟萃分析表明SCN5A(+)的心律失常事件风险高于SCN5A(-)。

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