基因型对长QT综合征临床病程的影响。国际长QT综合征注册研究组。

Influence of the genotype on the clinical course of the long-QT syndrome. International Long-QT Syndrome Registry Research Group.

作者信息

Zareba W, Moss A J, Schwartz P J, Vincent G M, Robinson J L, Priori S G, Benhorin J, Locati E H, Towbin J A, Keating M T, Lehmann M H, Hall W J

机构信息

Department of Medicine, University of Rochester School of Medicine and Dentistry, NY, USA.

出版信息

N Engl J Med. 1998 Oct 1;339(14):960-5. doi: 10.1056/NEJM199810013391404.

DOI:10.1056/NEJM199810013391404

PMID:9753711

Abstract

BACKGROUND

The congenital long-QT syndrome, caused by mutations in cardiac potassium-channel genes (KVLQT1 at the LQT1 locus and HERG at the LQT2 locus) and the sodium-channel gene (SCN5A at the LQT3 locus), has distinct repolarization patterns on electrocardiography, but it is not known whether the genotype influences the clinical course of the disease.

METHODS

We determined the genotypes of 541 of 1378 members of 38 families enrolled in the International Long-QT Syndrome Registry: 112 had mutations at the LQT1 locus, 72 had mutations at the LQT2 locus, and 62 had mutations at the LQT3 locus. We determined the cumulative probability and lethality of cardiac events (syncope, aborted cardiac arrest, or sudden death) occurring from birth through the age of 40 years according to genotype in the 246 gene carriers and in all 1378 members of the families studied.

RESULTS

The frequency of cardiac events was higher among subjects with mutations at the LQT1 locus (63 percent) or the LQT2 locus (46 percent) than among subjects with mutations at the LQT3 locus (18 percent) (P<0.001 for the comparison of all three groups). In a multivariate Cox analysis, the genotype and the QT interval corrected for heart rate were significant independent predictors of a first cardiac event. The cumulative mortality through the age of 40 among members of the three groups of families studied was similar; however, the likelihood of dying during a cardiac event was significantly higher (P<0.001) among families with mutations at the LQT3 locus (20 percent) than among those with mutations at the LQT1 locus (4 percent) or the LQT2 locus (4 percent).

CONCLUSIONS

The genotype of the long-QT syndrome influences the clinical course. The risk of cardiac events is significantly higher among subjects with mutations at the LQT1 or LQT2 locus than among those with mutations at the LQT3 locus. Although cumulative mortality is similar regardless of the genotype, the percentage of cardiac events that are lethal is significantly higher in families with mutations at the LQT3 locus.

摘要

背景

先天性长QT综合征由心脏钾通道基因（LQT1位点的KVLQT1和LQT2位点的HERG）及钠通道基因（LQT3位点的SCN5A）突变引起，在心电图上有不同的复极模式，但基因型是否影响疾病的临床病程尚不清楚。

方法

我们确定了国际长QT综合征注册研究中38个家系的1378名成员中541人的基因型：112人在LQT1位点有突变，72人在LQT2位点有突变，62人在LQT3位点有突变。我们根据246名基因携带者及所研究家系的所有1378名成员的基因型，确定了从出生到40岁发生心脏事件（晕厥、心脏骤停未遂或猝死）的累积概率和致死率。

结果

LQT1位点（63%）或LQT2位点（46%）有突变的受试者发生心脏事件的频率高于LQT3位点有突变的受试者（18%）（三组比较，P<0.001）。在多变量Cox分析中，基因型和经心率校正的QT间期是首次心脏事件的显著独立预测因素。所研究的三组家系成员到40岁时的累积死亡率相似；然而，LQT3位点有突变的家系（20%）在心脏事件期间死亡的可能性显著高于LQT1位点（4%）或LQT2位点（4%）有突变的家系（P<0.001）。