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MYBPC3基因中的一种新型奠基者突变:与西班牙最常见的MYBPC3突变的表型比较。

A Novel Founder Mutation in MYBPC3: Phenotypic Comparison With the Most Prevalent MYBPC3 Mutation in Spain.

作者信息

Sabater-Molina María, Saura Daniel, García-Molina Sáez Esperanza, González-Carrillo Josefa, Polo Luis, Pérez-Sánchez Inmaculada, Olmo María Del Carmen, Oliva-Sandoval María José, Barriales-Villa Roberto, Carbonell Pablo, Pascual-Figal Domigo, Gimeno Juan R

机构信息

Unidad de Cardiopatías Hereditarias, Hospital Universitario Virgen de la Arrixaca, El Palmar, Murcia, Spain.

Departamento de Cardiología, Hospital Universitario Virgen de la Arrixaca, El Palmar, Murcia, Spain.

出版信息

Rev Esp Cardiol (Engl Ed). 2017 Feb;70(2):105-114. doi: 10.1016/j.rec.2016.06.020. Epub 2016 Oct 28.

DOI:10.1016/j.rec.2016.06.020
PMID:28029522
Abstract

INTRODUCTION AND OBJECTIVES

Mutations in MYBPC3 are the cause of hypertrophic cardiomyopathy (HCM). Although most lead to a truncating protein, the severity of the phenotype differs. We describe the clinical phenotype of a novel MYBPC3 mutation, p.Pro108Alafs*9, present in 13 families from southern Spain and compare it with the most prevalent MYBPC3 mutation in this region (c.2308+1 G>A).

METHODS

We studied 107 relatives of 13 index cases diagnosed as HCM carriers of the p.Pro108Alafs*9 mutation. Pedigree analysis, clinical evaluation, and genotyping were performed.

RESULTS

A total of 54 carriers of p.Pro108Alafs9 were identified, of whom 39 had HCM. There were 5 cases of sudden death in the 13 families. Disease penetrance was greater as age increased and HCM patients were more frequently male and developed disease earlier than female patients. The phenotype was similar in p.Pro108Alafs9 and in c.2308+1 G>A, but differences were found in several risk factors and in survival. There was a trend toward a higher left ventricular mass in p.Pro108Alafs*9 vs c.2308+1G>A. Cardiac magnetic resonance revealed a similar extent and pattern of fibrosis.

CONCLUSIONS

The p.Pro108Alafs*9 mutation is associated with HCM, high penetrance, and disease onset in middle age.

摘要

引言与目的

MYBPC3基因突变是肥厚型心肌病(HCM)的病因。尽管大多数突变会导致截短蛋白,但表型的严重程度有所不同。我们描述了一种新型MYBPC3突变p.Pro108Alafs*9的临床表型,该突变存在于西班牙南部的13个家族中,并将其与该地区最常见的MYBPC3突变(c.2308+1 G>A)进行比较。

方法

我们研究了13例被诊断为携带p.Pro108Alafs*9突变的HCM先证者的107名亲属。进行了系谱分析、临床评估和基因分型。

结果

共鉴定出54名p.Pro108Alafs9突变携带者,其中39人患有HCM。13个家族中有5例猝死。随着年龄增长,疾病外显率增加,HCM患者男性更为常见,且发病早于女性患者。p.Pro108Alafs9和c.2308+1 G>A的表型相似,但在一些危险因素和生存率方面存在差异。与c.2308+1 G>A相比,p.Pro108Alafs*9的左心室质量有升高趋势。心脏磁共振成像显示纤维化程度和模式相似。

结论

p.Pro108Alafs*9突变与HCM、高外显率和中年发病有关。

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