Association between mutation status and left ventricular reverse remodelling in dilated cardiomyopathy

医学 射血分数 扩张型心肌病 LMNA公司 内科学 心脏病学 基因突变 突变 基因 遗传学 病理 生物 心力衰竭
作者
Matteo Dal Ferro,Davide Stolfo,Alessandro Altinier,Marta Gigli,Martina Perrieri,Federica Ramani,Giulia Barbati,Alberto Pivetta,Francesca Brun,Lorenzo Monserrat,Mauro Giacca,Luisa Mestroni,Marco Merlo,Gianfranco Sinagra
出处
期刊:Heart [BMJ]
卷期号:103 (21): 1704-1710 被引量:89
标识
DOI:10.1136/heartjnl-2016-311017
摘要

Objective To explore the genetic landscape of a well selected dilated cardiomyopathy (DCM) cohort, assessing the possible relation between different genotypes and left ventricular reverse remodelling (LVRR). Methods A cohort of 152 patients with DCM from the Heart Muscle Disease Registry of Trieste has been studied by next-generation sequencing (NGS). Patients were grouped into different ‘gene-clusters’ with functionally homogeneous genetic backgrounds. LVRR was defined by left ventricular ejection fraction normalisation or increase ≥10% associated with normalisation in indexed left ventricular end-diastolic diameter or relative decrease ≥10% at 24 months follow-up. Results A pathogenic disease-related gene variant was identified in 57% of patients: 28 (18%) TTN ; 7 (5%) LMNA ; 16 (11%) structural cytoskeleton Z-disk genes; 9 (6%) desmosomal genes; 18 (12%) motor sarcomeric genes and 9 (6%) other genes. Baseline clinical features were similar throughout the different genotypes. A significant relationship was found between gene cluster subgroups and LVRR, with a lower rate of LVRR in structural cytoskeleton Z-disk gene mutation carriers (1/16 patients, 6%, p<0.05 vs the other subgroups). Of note, structural cytoskeleton Z-disk gene rare variants were independently and inversely associated with LVRR when adjusted for clinical predictors of LVRR (OR 0.065; 95% CI 0.008 to 0.535, p=0.011). Conclusions NGS confirmed a high genetic diagnostic yield in DCM. A specific ‘gene-clusters’ classification based on functional similarities in different genes might be helpful in the clinical management of genetically determined DCM. In this study, structural cytoskeleton Z-disk gene rare variants were independently associated with a lower rate of LVRR at follow-up.
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