Pasotti Michele, Klersy Catherine, Pilotto Andrea, Marziliano Nicola, Rapezzi Claudio, Serio Alessandra, Mannarino Savina, Gambarin Fabiana, Favalli Valentina, Grasso Maurizia, Agozzino Manuela, Campana Carlo, Gavazzi Antonello, Febo Oreste, Marini Massimiliano, Landolina Maurizio, Mortara Andrea, Piccolo Giovanni, Viganò Mario, Tavazzi Luigi, Arbustini Eloisa
Centre for Inherited Cardiovascular Diseases, Molecular Diagnostic Laboratory, Fondazione IRCCS Policlinico San Matteo, Pavia, Italy.
J Am Coll Cardiol. 2008 Oct 7;52(15):1250-60. doi: 10.1016/j.jacc.2008.06.044.
The aim of this study was to analyze the long-term follow-up of dilated cardiolaminopathies.
Lamin A/C (LMNA) gene mutations cause a variety of phenotypes. In the cardiology setting, patients diagnosed with idiopathic dilated cardiomyopathy (DCM) plus atrioventricular block (AVB) constitute the majority of reported cases.
Longitudinal retrospective observational studies were conducted with 27 consecutive families in which LMNA gene defects were identified in the probands, all sharing the DCM phenotype.
Of the 164 family members, 94 had LMNA gene mutations. Sixty of 94 (64%) were phenotypically affected whereas 34 were only genotypically affected, including 5 with pre-clinical signs. Of the 60 patients, 40 had DCM with AVB, 12 had DCM with ventricular tachycardia/fibrillation, 6 had DCM with AVB and Emery-Dreifuss muscular dystrophy type 2 (EDMD2), and 2 had AVB plus EDMD2. During a median of 57 months (interquartile range 36 to 107 months), we observed 49 events in 43 DCM patients (6 had a later event, excluded from the analysis). The events were related to heart failure (15 heart transplants, 1 death from end-stage heart failure) and ventricular arrhythmias (15 sudden cardiac deaths and 12 appropriate implantable cardioverter-defibrillator interventions). By multivariable analysis, New York Heart Association functional class III to IV and highly dynamic competitive sports for >or=10 years were independent predictors of total events. By a bivariable Cox model, splice site mutations and competitive sport predicted sudden cardiac death.
Dilated cardiomyopathies caused by LMNA gene defects are highly penetrant, adult onset, malignant diseases characterized by a high rate of heart failure and life-threatening arrhythmias, predicted by New York Heart Association functional class, competitive sport activity, and type of mutation.
本研究旨在分析扩张型心肌病的长期随访情况。
核纤层蛋白A/C(LMNA)基因突变会导致多种表型。在心脏病学领域,被诊断为特发性扩张型心肌病(DCM)加房室传导阻滞(AVB)的患者构成了大多数报告病例。
对连续27个家系进行纵向回顾性观察研究,这些家系的先证者中均鉴定出LMNA基因缺陷,所有家系成员均具有DCM表型。
在164名家庭成员中,94人有LMNA基因突变。94人中60人(64%)有表型影响,34人仅有基因型影响,其中5人有临床前体征。在60例患者中,40例患有DCM合并AVB,12例患有DCM合并室性心动过速/颤动,6例患有DCM合并AVB和2型埃默里-德赖富斯肌营养不良症(EDMD2),2例患有AVB加EDMD2。在中位57个月(四分位间距36至107个月)期间,我们在43例DCM患者中观察到49起事件(6例有较晚发生的事件,排除在分析之外)。这些事件与心力衰竭(15例心脏移植,1例死于终末期心力衰竭)和室性心律失常(15例心源性猝死和12例适当的植入式心脏复律除颤器干预)有关。通过多变量分析,纽约心脏协会功能分级III至IV级以及从事≥10年的高强度竞技运动是总事件的独立预测因素。通过双变量Cox模型,剪接位点突变和竞技运动可预测心源性猝死。
由LMNA基因缺陷引起的扩张型心肌病具有高度外显率,成年发病,是恶性疾病,其特征为心力衰竭发生率高和危及生命的心律失常,可由纽约心脏协会功能分级、竞技运动活动和突变类型预测。
