Hypertrophic cardiomyopathy due to truncating variants in myosin binding protein C: a Spanish cohort.

IF 2.8 Q2 CARDIAC & CARDIOVASCULAR SYSTEMS
Maria Melendo-Viu, Rafael Salguero-Bodes, María Valverde-Gómez, Jose María Larrañaga-Moreira, Roberto Barriales, Carles Díez-Lopez, Javier Limeres Freire, Maria Luisa Peña-Peña, Pablo Garcia Pavia, Tomas Ripoll, Vicente Climent-Payá, Maria Gallego Delgado, Esther Zorio, Francisco José Bermudez Jimenez, José Manuel García-Pinilla, Irene Méndez Fernández, Maria Sabater-Molina, Ana Perez Asensio, Álvaro Marchán-Lopez, Fernando Arribas Ynsaurriaga, Hector Bueno, Julián A Palomino Doza
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引用次数: 0

Abstract

Background: Hypertrophic cardiomyopathy (HCM) is an inherited disorder whose causal variants involve sarcomeric protein genes. One of these is myosin-binding protein C (MYBPC3), being previously associated with a favourable prognosis. Our objective is to describe the clinical characteristics and events of a molecularly homogeneous HCM cohort associated with truncating MYBPC3 variants.

Methods and results: A cohort of patients and relatives with HCM diagnosis and carrying a truncating MYBPC3 variant were retrospectively recruited. Subjects had an average follow-up of 7.77 years, with an incident HCM phenotype of 10%. They were middle-aged adult patients (47±16.8 years) without significant comorbidities or symptoms. Hypertrophy was discrete with a significative difference between probands and relatives (17.5±4 mm vs 14.6±5 mm; p<0.0001). Ejection fraction was predominantly preserved (65%±10%). Despite it being the most common clinical event, relevant heart failure (observed in 8.1% of patients) was infrequent and commonly found in the presence of a second environmental precipitating agent. ESC-HCM risk calculator and modifier factors did not correlate with the risk of major events predicting events, which were low (1.51 per 100 patients/year) and associated with the severity of HCM, abnormal QRS in the ECG and age. Genetic factors and sex were not associated with major events.

Conclusions: This is the first molecularly homogeneous, contemporary cohort, including HCM patients secondary to MYBPC3 truncating variants. Patients showed a good prognosis with a low event rate. In our cohort, major arrhythmic events were not related to measured environmental or genetic factors.

肌球蛋白结合蛋白 C 截短变异导致的肥厚型心肌病:西班牙队列。
背景:肥厚型心肌病(HCM)是一种遗传性疾病,其病因变异涉及肌纤维蛋白基因。其中一个基因是肌球蛋白结合蛋白 C(MYBPC3),它曾与良好的预后有关。我们的目的是描述与截短的 MYBPC3 变异相关的分子同质性 HCM 群体的临床特征和事件:我们回顾性地招募了一批确诊为 HCM 并携带截短 MYBPC3 变体的患者及其亲属。受试者的平均随访时间为 7.77 年,HCM 表型发生率为 10%。他们都是中年成人患者(47±16.8 岁),没有明显的合并症或症状。肥大是不连续的,原发者和亲属之间存在显著差异(17.5±4 mm vs 14.6±5 mm; p结论:这是首个分子同质的现代队列,包括继发于 MYBPC3 截断变异的 HCM 患者。患者预后良好,事件发生率低。在我们的队列中,主要心律失常事件与测量的环境或遗传因素无关。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Open Heart
Open Heart CARDIAC & CARDIOVASCULAR SYSTEMS-
CiteScore
4.60
自引率
3.70%
发文量
145
审稿时长
20 weeks
期刊介绍: Open Heart is an online-only, open access cardiology journal that aims to be “open” in many ways: open access (free access for all readers), open peer review (unblinded peer review) and open data (data sharing is encouraged). The goal is to ensure maximum transparency and maximum impact on research progress and patient care. The journal is dedicated to publishing high quality, peer reviewed medical research in all disciplines and therapeutic areas of cardiovascular medicine. Research is published across all study phases and designs, from study protocols to phase I trials to meta-analyses, including small or specialist studies. Opinionated discussions on controversial topics are welcomed. Open Heart aims to operate a fast submission and review process with continuous publication online, to ensure timely, up-to-date research is available worldwide. The journal adheres to a rigorous and transparent peer review process, and all articles go through a statistical assessment to ensure robustness of the analyses. Open Heart is an official journal of the British Cardiovascular Society.
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