多中心临床和功能证据重新分类了一种复发性非典型细丝蛋白 C 剪接改变变体。
Multicenter clinical and functional evidence reclassifies a recurrent noncanonical filamin C splice-altering variant.
机构信息
Vanderbilt University School of Medicine, Medical Scientist Training Program, Vanderbilt University, Nashville, Tennessee.
Cardiovascular Institute and Adult Medical Genetics Program, University of Colorado Anschutz Medical Campus, Aurora, Colorado.
出版信息
Heart Rhythm. 2023 Aug;20(8):1158-1166. doi: 10.1016/j.hrthm.2023.05.006. Epub 2023 May 9.
BACKGROUND
Truncating variants in filamin C (FLNC) can cause arrhythmogenic cardiomyopathy (ACM) through haploinsufficiency. Noncanonical splice-altering variants may contribute to this phenotype.
OBJECTIVE
The purpose of this study was to investigate the clinical and functional consequences of a recurrent FLNC intronic variant of uncertain significance (VUS), c.970-4A>G.
METHODS
Clinical data in 9 variant heterozygotes from 4 kindreds were obtained from 5 tertiary health care centers. We used in silico predictors and functional studies with peripheral blood and patient-specific induced pluripotent stem cell-derived cardiomyocytes (iPSC-CMs). Isolated RNA was studied by reverse transcription polymerase chain reaction. iPSC-CMs were further characterized at baseline and after nonsense-mediated decay (NMD) inhibition, using quantitative polymerase chain reaction (qPCR), RNA-sequencing, and cellular electrophysiology. American College of Medical Genetics and Genomics (ACMG) criteria were used to adjudicate variant pathogenicity.
RESULTS
Variant heterozygotes displayed a spectrum of disease phenotypes, spanning from mild ventricular dysfunction with palpitations to severe ventricular arrhythmias requiring device shocks or progressive cardiomyopathy requiring heart transplantation. Consistent with in silico predictors, the c.970-4A>G FLNC variant activated a cryptic splice acceptor site, introducing a 3-bp insertion containing a premature termination codon. NMD inhibition upregulated aberrantly spliced transcripts by qPCR and RNA-sequencing. Patch clamp studies revealed irregular spontaneous action potentials, increased action potential duration, and increased sodium late current in proband-derived iPSC-CMs. These findings fulfilled multiple ACMG criteria for pathogenicity.
CONCLUSION
Clinical, in silico, and functional evidence support the prediction that the intronic c.970-4A>G VUS disrupts splicing and drives ACM, enabling reclassification from VUS to pathogenic.
背景
细丝蛋白 C (FLNC) 的截断变异可通过杂合不足导致致心律失常性心肌病 (ACM)。非规范剪接改变变异可能对此表型有贡献。
目的
本研究旨在探讨一个不确定意义的 FLNC 内含子变异体 c.970-4A>G 的临床和功能后果。
方法
从 5 家三级保健中心的 4 个家系中获得了 9 个变异杂合子的临床数据。我们使用了计算机预测和功能研究,使用外周血和患者特异性诱导多能干细胞衍生的心肌细胞 (iPSC-CMs)。通过逆转录聚合酶链反应研究分离的 RNA。在使用无意义介导的衰变 (NMD) 抑制后,通过定量聚合酶链反应 (qPCR)、RNA 测序和细胞电生理学进一步对 iPSC-CMs 进行了特征分析。美国医学遗传学与基因组学学院 (ACMG) 标准用于裁决变异的致病性。
结果
变异杂合子表现出从轻度心室功能障碍伴心悸到需要心脏除颤器电击的严重室性心律失常,再到需要心脏移植的进行性心肌病等一系列疾病表型。与计算机预测一致,c.970-4A>G FLNC 变异激活了一个隐蔽的剪接受体位点,引入了一个包含提前终止密码子的 3 个碱基插入。NMD 抑制通过 qPCR 和 RNA 测序上调了异常剪接的转录本。膜片钳研究显示,在源自先证者的 iPSC-CMs 中,不规则的自发性动作电位、动作电位持续时间延长和钠离子晚期电流增加。这些发现满足了 ACMG 多个致病性标准。
结论
临床、计算机和功能证据支持这样的预测,即内含子 c.970-4A>G 变异破坏了剪接并导致 ACM,从而使该变异从意义不明的变异体 (VUS) 重新分类为致病性。
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