Kolokotronis Konstantinos, Pluta Natalie, Klopocki Eva, Kunstmann Erdmute, Messroghli Daniel, Maack Christoph, Tejman-Yarden Shai, Arad Michael, Rost Simone, Gerull Brenda
Institute of Human Genetics, Biocenter, Julius-Maximilians-University Würzburg, 97074 Würzburg, Germany.
German Heart Center Berlin, Department of Internal Medicine-Cardiology, 13353 Berlin, Germany.
J Clin Med. 2020 Jul 9;9(7):2168. doi: 10.3390/jcm9072168.
Inherited cardiomyopathies are characterized by clinical and genetic heterogeneity that challenge genetic diagnostics. In this study, we examined the diagnostic benefit of exome data compared to targeted gene panel analyses, and we propose new candidate genes. We performed exome sequencing in a cohort of 61 consecutive patients with a diagnosis of cardiomyopathy or primary arrhythmia, and we analyzed the data following a stepwise approach. Overall, in 64% of patients, a variant of interest (VOI) was detected. The detection rate in the main sub-cohort consisting of patients with dilated cardiomyopathy (DCM) was much higher than previously reported (25/36; 69%). The majority of VOIs were found in disease-specific panels, while a further analysis of an extended panel and exome data led to an additional diagnostic yield of 13% and 5%, respectively. Exome data analysis also detected variants in candidate genes whose functional profile suggested a probable pathogenetic role, the strongest candidate being a truncating variant in In conclusion, although the diagnostic yield of gene panels is acceptable for routine diagnostics, the genetic heterogeneity of cardiomyopathies and the presence of still-unknown causes favor exome sequencing, which enables the detection of interesting phenotype-genotype correlations, as well as the identification of novel candidate genes.
遗传性心肌病具有临床和遗传异质性,这给基因诊断带来了挑战。在本研究中,我们比较了外显子组数据与靶向基因panel分析的诊断效益,并提出了新的候选基因。我们对61例连续诊断为心肌病或原发性心律失常的患者进行了外显子组测序,并采用逐步方法分析数据。总体而言,在64%的患者中检测到了感兴趣的变异(VOI)。主要亚组中扩张型心肌病(DCM)患者的检测率远高于先前报道(25/36;69%)。大多数VOI在疾病特异性panel中被发现,而对扩展panel和外显子组数据的进一步分析分别导致了13%和5%的额外诊断率。外显子组数据分析还在候选基因中检测到变异,其功能特征表明可能具有致病作用,最有力的候选基因是一个截短变异。总之,尽管基因panel的诊断率对于常规诊断是可接受的,但心肌病的遗传异质性和仍未知原因的存在有利于外显子组测序,其能够检测到有趣的表型-基因型相关性,以及鉴定新的候选基因。