Clinical and genetic characterization of patients with catecholaminergic polymorphic ventricular tachycardia: a case series

S. Komissarova, N. Rineiska, N. Chakova, S. Niyazova, L. Plashchinskaya, Veronika Ch. Barsukevich, Olga V. Podpalova
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Abstract

AIM: of the study was to evaluate the clinical and genetic characteristics, including the development of adverse events and outcomes in patients with catecholaminergic polymorphic ventricular tachycardia (CPVT). MATERIALS AND METHODS: The clinical phenotype of eight patients with CPVT, two of whom were relatives of probands, was observed over 4 years. The clinical and instrumental study included ECG-12, 24-hour Holter ECG monitoring, genealogical history collection and family history of sudden cardiac death (SCD), transthoracic echocardiography and cardiac magnetic resonance imaging to detect structural myocardial changes, electrophysiologic study according to indications, and ICD monitoring. High-throughput sequencing (NGS) was utilized to search for mutations in genes linked to the onset of channelopathies and other inherited rhythm disorders. RESULTS: In 8 patients, nucleotide variants of pathogenicity classes III-V were identified according to the ACMG (2015) criteria in the RYR2 gene associated with CPVT. Pathogenic (IV-V class) and likely pathogenic (IV class) mutations in the RYR2 gene were found in 6 (75%) probands, variants with uncertain clinical significance (VUS, class III) were found in 2 patients. At the time of diagnosis, transient QTc interval prolongation of more than 480 ms was detected in 4 (50%) patients; bradycardia less than 54 beats/min — in 2 (25%) patients, sequences of supraventricular tachycardia and ventricular tachyarrhythmia — in 2 (25%) patients. The most severe form of the disease with marked clinical manifestations and an episode of clinical death with subsequent resuscitation, as well as a transient QTc interval prolongation exceeding 500 ms was observed in patients with mutations c.11814C A (p.Ser3938Arg, rs794728704); c.463G A (p.Gly155Arg) and c.14876G A (p.Arg4959Gln, rs794728811) in the RYR2 gene. Three (37.5%) patients underwent ICD implantation; one for primary SCD prevention and two for secondary prevention. CONCLUSION: In this study, the spectrum of clinical manifestations in patients with genetically confirmed CPVT was examined. The findings highlight transient QTc interval extensions, significant sinus bradycardia, and sequences of supraventricular tachyarrhythmias, which can escalate into life-threatening ventricular tachyarrhythmias in CPVT patients.
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儿茶酚胺能多态性室性心动过速患者的临床和遗传特征:一个病例系列
研究目的:评估儿茶酚胺能多形性室性心动过速(CPVT)患者的临床和遗传特征,包括不良事件的发生和结局。材料与方法:对 8 名 CPVT 患者的临床表型进行了长达 4 年的观察,其中 2 人是原发性 CPVT 患者的亲属。临床和仪器研究包括心电图(ECG-12)、24 小时 Holter 心电图监测、家谱史收集和心脏性猝死(SCD)家族史、经胸超声心动图和心脏磁共振成像以检测心肌结构变化、根据适应症进行电生理研究和 ICD 监测。利用高通量测序(NGS)寻找与通道病和其他遗传性心律失常发病有关的基因突变。结果:根据 ACMG(2015 年)标准,在 8 例患者中发现了与 CPVT 相关的 RYR2 基因中 III-V 类致病性核苷酸变异。在 6 名(75%)患者中发现了 RYR2 基因的致病性(IV-V 级)和可能致病性(IV 级)变异,在 2 名患者中发现了临床意义不确定的变异(VUS,III 级)。在确诊时,4 名患者(50%)的 QTc 间期一过性延长超过 480 毫秒;2 名患者(25%)的心动过缓低于 54 次/分,2 名患者(25%)出现室上性心动过速和室性心动过速。在 RYR2 基因突变为 c.11814C A(p.Ser3938Arg,rs794728704)、c.463G A(p.Gly155Arg)和 c.14876G A(p.Arg4959Gln,rs794728811)的患者中,观察到了最严重的疾病形式,临床表现明显,并在随后的抢救中出现临床死亡,以及一过性 QTc 间期延长超过 500 毫秒。三名(37.5%)患者接受了 ICD 植入术;其中一名用于 SCD 一级预防,两名用于二级预防。结论:本研究探讨了经基因证实的 CPVT 患者的临床表现谱。研究结果表明,CPVT 患者会出现一过性 QTc 间期延长、明显的窦性心动过缓和室上性快速性心律失常序列,这些症状可升级为危及生命的室性快速性心律失常。
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