Meregalli Paola G, Tan Hanno L, Probst Vincent, Koopmann Tamara T, Tanck Michael W, Bhuiyan Zahurul A, Sacher Frederic, Kyndt Florence, Schott Jean-Jacques, Albuisson J, Mabo Philippe, Bezzina Connie R, Le Marec Herve, Wilde Arthur A M
Department of Cardiology, Academic Medical Centre, University of Amsterdam, Amsterdam, the Netherlands.
Heart Rhythm. 2009 Mar;6(3):341-8. doi: 10.1016/j.hrthm.2008.11.009. Epub 2008 Nov 11.
Patients carrying loss-of-function SCN5A mutations linked to Brugada syndrome (BrS) or progressive cardiac conduction disease (PCCD) are at risk of sudden cardiac death at a young age. The penetrance and expressivity of the disease are highly variable, and new tools for risk stratification are needed.
We aimed to establish whether the type of SCN5A mutation correlates with the clinical and electrocardiographic phenotype.
We studied BrS or PCCD probands and their relatives who carried a SCN5A mutation. Mutations were divided into 2 main groups: missense mutations (M) or mutations leading to premature truncation of the protein (T). The M group was subdivided according to available biophysical properties: M mutations with <or=90% (M(active)) or >90% (M(inactive)) peak I(Na) reduction were analyzed separately.
The study group was composed of 147 individuals with 32 different mutations. No differences in age and sex distribution were found between the groups. Subjects carrying a T mutation had significantly more syncopes than those with an M(active) mutation (19 of 75 versus 2 of 35, P = .03). Also, mutations associated with drastic peak I(Na) reduction (T and M(inactive) mutants) had a significantly longer PR interval, compared with M(active) mutations. All other electrocardiographic parameters were comparable. After drug provocation testing, both PR and QRS intervals were significantly longer in the T and M(inactive) groups than in the M(active) group.
In loss-of-function SCN5A channelopathies, patients carrying T and M(inactive) mutations develop a more severe phenotype than those with M(active) mutations. This is associated with more severe conduction disorders. This is the first time that genetic data are proposed for risk stratification in BrS.
携带与Brugada综合征(BrS)或进行性心脏传导疾病(PCCD)相关的功能丧失型SCN5A突变的患者在年轻时有心脏性猝死的风险。该疾病的外显率和表现度高度可变,因此需要新的风险分层工具。
我们旨在确定SCN5A突变类型是否与临床和心电图表型相关。
我们研究了携带SCN5A突变的BrS或PCCD先证者及其亲属。突变分为2个主要组:错义突变(M)或导致蛋白质过早截断的突变(T)。M组根据可用的生物物理特性进一步细分:分别分析钠电流(I Na)峰值降低≤90%(M(活性))或>90%(M(非活性))的M突变。
研究组由147名携带32种不同突变的个体组成。各组之间在年龄和性别分布上未发现差异。携带T突变的受试者晕厥明显多于携带M(活性)突变的受试者(75例中有19例,35例中有2例,P = 0.03)。此外,与M(活性)突变相比,与I Na峰值大幅降低相关的突变(T和M(非活性)突变体)的PR间期明显更长。所有其他心电图参数相当。药物激发试验后,T组和M(非活性)组的PR和QRS间期均明显长于M(活性)组。
在功能丧失型SCN5A通道病中,携带T和M(非活性)突变的患者比携带M(活性)突变的患者表现出更严重的表型。这与更严重的传导障碍有关。这是首次提出用于BrS风险分层的遗传数据。
