儿童RYR2基因变异相关儿茶酚胺敏感性多形性室性心动过速诊治及随访分析

doi:10.12372/jcp.2024.23e0983

Abstract

Abstract:

Objective To investigate the clinical manifestations, treatment and follow-up of RYR2 gene variation-related catecholaminergic polymorphic ventricular tachycardia (CPVT). Methods The clinical data of CPVT children admitted from January 2017 to January 2023 were retrospectively analyzed, and the course of treatment and follow-up results were summarized. Results A total of 6 children (4 boys and 2 girls) with CPVT were admitted, and the mean age of the patients was (3.5±0.5) years old when the first symptoms appeared. The median time from first symptom onset to diagnosis was 1.5 (0.1-5.9) years. The most common clinical manifestation was syncope, with exercise and emotions being the main triggers. All 6 children had de novo missense mutations in the RYR2 gene identified through whole-exome sequencing. In dynamic electrocardiography, atrial arrhythmias and sinoatrial node dysfunction were commonly observed in younger children. Four patients underwent exercise stress testing, with 2 experiencing bidirectional ventricular premature contractions and 2 experiencing bidirectional ventricular premature contractions and polymorphic ventricular tachycardia. Initial treatment involved oral propranolol or metoprolol. If arrhythmias persisted, flecainide or propafenone was added as adjunctive therapy. Two patients received permanent cardiac pacemaker treatment (VVI). The mean follow-up time was (24.3±3.7) months, and all patients survived. During the follow-up period, 3 children had occasional syncope, 1 had intermittent palpitation, and 2 had no discomfort. Conclusions CPVT associated with RYR2 gene variations in children can present with various clinical manifestations. Atrial arrhythmias combined with sinoatrial node dysfunction are commonly observed in younger children. The combination of pharmacological therapy and cardiac pacemaker treatment yields favorable treatment outcomes.

Key words: RYR2 gene, catecholaminergic polymorphic ventricular tachycardia, child

WANG Yefeng, ZENG Min, XIAO Yunbin, WANG Xiang, CHEN Zhi. Clinical characteristics and follow-up of catecholaminergic polymorphic ventricular tachycardia associated with RYR2 gene variation in children[J].Journal of Clinical Pediatrics, 2024, 42(10): 857-862.

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References 20

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患儿	性别	首发年龄/岁	确诊年龄/岁	首发诊断	晕厥	诱因	心电图	动态心电图	彩色多普勒超声心动图	运动平板	治疗方案	随访时间/月	随访期间表现
例1	女	2.6	11	室上性心动过速	有	运动	房速	房速、窦性停搏、短阵多源室速	左室增大EF正常	双向室早、多形室速	普萘洛尔(1.5mg·kg^-1·d^-1)，普罗帕酮(5 mg·kg^-1·d^-1)	37	晕厥2次
例2	男	5	6.9	癫痫	有	情绪激动	正常	阵发性房速、单源室早、窦缓	房间隔缺损	双向室早、多形室速	美托洛尔(1 mg·kg^-1·d^-1)后改为普萘洛尔(2 mg·kg^-1·d^-1)，VVI心内膜起搏	28	间断心悸
例3	男	2.6	2.7	心肌炎	无	无	房速	房速、房扑、房颤、窦性停搏	全心增大EF减低	未做	普萘洛尔(1.5 mg·kg^-1·d^-1)，氟卡尼(2 mg·kg^-1·d^-1)，VVI心外膜起搏	30	晕厥1次
例4	男	4	9	癫痫	有	运动	V2导联T波切迹	双源室早	正常	双向室早	普萘洛尔(2mg·kg^-1·d^-1)	20	无不适
例5	女	2	2.1	心肌炎	无	无	房速、房扑	房速、房扑、窦缓、QT延长	左室增大EF减低	未做	普萘洛尔(2mg·kg^-1·d^-1)	12	无不适
例6	男	5	6	癫痫	有	运动	偶发房早，V2导联T波切迹	交界性心动过速、多源室早	正常	双向室早	美托洛尔(1 mg·kg^-1·d^-1)后改为普萘洛尔(2 mg·kg^-1·d^-1)	19	晕厥1次

患儿	基因	遗传方式	合子状态	突变类型	核苷酸改变	氨基酸改变	变异来源	ACMG评级	评级依据
例1	RYR2	AD	杂合	错义	c.14311G>A	p.V4771I	新发	可能致病	PM2-P+PP3-A1+PP3-B1+PS4-M+PP2+PM6
例2	RYR2	AD	杂合	错义	c.12534C>A	p.N4178K	新发	可能致病	PM2-P+PP3-A1+PP3-B2+PM1+PP2+PM6
例3	RYR2	AD	杂合	错义	c.12515T>A	p.F4172Y	新发	可能致病	PM2-P+PP3-A1+PP3-B1+PM5+ PP2+PS2
例4	RYR2	AD	杂合	错义	c.536A>G	p.D179G	新发	可能致病	PM2-P+PP3-A1+PP3-S+PM1+PP2+PM6
例5	RYR2	AD	杂合	错义	c.11997G>A	p.M3999I	新发	可能致病	PM2-P+PP3-A1+PP3-B1+PM5+ PP2+PS2
例6	RYR2	AD	杂合	错义	c.41T>G	p.L14R	新发	可能致病	PM2-P+PP3-A1+PP3-B1-M+PM5+PS2

Clinical characteristics and follow-up of catecholaminergic polymorphic ventricular tachycardia associated with RYR2 gene variation in children

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