一名9岁儿童因RYR2基因c.7580T>G突变导致儿茶酚胺能多形性室性心动过速延迟诊断6年。
A delayed diagnosis of catecholaminergic polymorphic ventricular tachycardia with a mutant of RYR2 at c.7580T>G for 6 years in a 9-year-old child.
作者信息
Duan Hongyu, Lu Yongyi, Yan Song, Qiao Lina, Hua Yimin, Li Yifei, Zhou Kaiyu, Wang Chuan
机构信息
Department of Pediatrics, West China Second University Hospital, Sichuan University The Cardiac Development and Early Intervention Unit, West China Institute of Women and Children's Health, West China Second University Hospital, Sichuan University Key Laboratory of Birth Defects and Related Diseases of Women and Children (Sichuan University), Ministry of Education, Chengdu, Sichuan, China.
出版信息
Medicine (Baltimore). 2018 Apr;97(16):e0368. doi: 10.1097/MD.0000000000010368.
RATIONALE
Catecholaminergic polymorphic ventricular tachycardia (CPVT) is a rare but potentially lethal inherited arrhythmia syndrome induced by adrenergic stress. Due to the atypical clinical manifestations in early age, limited recognition and experience of pediatric cardiologists, and low awareness of the significance of genetic diagnosis in some underdeveloped areas in China, a delayed or missed diagnosis of CPVT in children is common and concerning.
PATIENT CONCERNS
A 9-year and 3-month male child with recurrent exercise-induced syncope accompanied by convulsion was initially misdiagnosed as epilepsy since the first manifestation at the age of 3 years. Due to the identification of polymorphic ventricular premature beats, nonsustained ventricular tachycardia (VT), and supraventricular tachycardia, a cardiogenic etiology was established. The patient received a successive treatment by propafenone, amiodarone, a combination of amiodarone with metoprolol, and metoprolol alone for up to 6 years.
DIAGNOSES
Given the poor response to conventional antiarrhythmics, excise-induced syncope, QRS morphology and a structurally normal heart, the diagnosis of CPVT was suspected, and ultimately confirmed by detection of polymorphic and bidirectional VT with degeneration into ventricular fibrillation during exercise testing. In addition, a heterozygous mutant of RYR2 at c.7580T > G was identified by genetic testing.
INTERVENTIONS
Due to the unavailability of flecainide in China and the refusal of implantable cardioverter defibrillator implantation by his parents, this patient continued to be treated with oral metoprolol.
OUTCOMES
Unfortunately, the effect was unfavorable during 4 months outpatient follow-up.
LESSONS
CPVT should be suspected in young patients with a normal baseline electrocardiogram (EKG), a structurally normal heart and polymorphic and/or bidirectional ventricular tachycardia induced by exercise or emotional stress. Exercise and genetic testing is essential and significant for a timely and accurate diagnosis of CPVT. The current study firstly reported a case with CPVT associated with a mutant of RYR2 at c.7580T > G in children.
理论依据
儿茶酚胺能多形性室性心动过速(CPVT)是一种由肾上腺素能应激诱发的罕见但潜在致命的遗传性心律失常综合征。由于其在儿童早期的临床表现不典型、儿科心脏病专家的认知和经验有限,以及中国一些欠发达地区对基因诊断重要性的认识不足,儿童CPVT的诊断延迟或漏诊很常见且令人担忧。
患者情况
一名9岁3个月的男性儿童,自3岁首次出现症状以来,反复出现运动诱发的晕厥并伴有抽搐,最初被误诊为癫痫。由于发现了多形性室性早搏、非持续性室性心动过速(VT)和室上性心动过速,确定了心源性病因。该患者先后接受了普罗帕酮、胺碘酮、胺碘酮与美托洛尔联合治疗以及单独使用美托洛尔治疗,长达6年。
诊断
鉴于对传统抗心律失常药物反应不佳、晕厥由运动诱发、QRS波形态以及心脏结构正常,怀疑为CPVT,并最终通过运动试验检测到多形性和双向性VT并恶化为心室颤动而确诊。此外,基因检测鉴定出RYR2基因c.7580T>G位点的杂合突变。
干预措施
由于中国无法获得氟卡尼,且其父母拒绝植入植入式心脏复律除颤器,该患者继续接受口服美托洛尔治疗。
结果
不幸的是,在4个月的门诊随访期间效果不佳。
经验教训
对于基线心电图(EKG)正常、心脏结构正常且运动或情绪应激诱发多形性和/或双向性室性心动过速的年轻患者,应怀疑CPVT。运动和基因检测对于CPVT的及时准确诊断至关重要。本研究首次报道了一例儿童CPVT与RYR2基因c.7580T>G突变相关的病例。
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