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Severe cardiac phenotype with right ventricular predominance in a large cohort of patients with a single missense mutation in the DES gene

医学 结蛋白 错义突变 物候学 致心律失常性右心室发育不良 心肌病 普氏球蛋白 心脏病学 表型 内科学 限制性心肌病 突变 移码突变 病理 遗传学 心力衰竭 生物 基因 波形蛋白 免疫组织化学 Wnt信号通路 连环素
作者
J. Peter van Tintelen,Isabelle C Van Gelder,Angeliki Asimaki,Albert J.H. Suurmeijer,Ans C.P. Wiesfeld,Jan D.H. Jongbloed,Arthur van den Wijngaard,Jan B. M. Kuks,Karin Y. van Spaendonck‐Zwarts,Nicolette C. Notermans,Ludolf G. Boven,Freek van den Heuvel,Hermine E. Veenstra‐Knol,Jeffrey E. Saffitz,Robert M.W. Hofstra,Maarten P. van den Berg
出处
期刊:Heart Rhythm [Elsevier BV]
卷期号:6 (11): 1574-1583 被引量:162
标识
DOI:10.1016/j.hrthm.2009.07.041
摘要

Desmin-related myopathy is a clinically heterogenous group of disorders encompassing myopathies, cardiomyopathies, conduction disease, and combinations of these disorders. Mutations in the gene encoding desmin (DES), a major intermediate filament protein, can underlie this phenotype.The purpose of this study was to investigate the clinical and pathologic characteristics of 27 patients from five families with an identical mutation in the head domain region (p.S13F) of desmin.All 27 carriers or obligate carriers of a p.S13F DES founder mutation demonstrated a fully penetrant yet variable phenotype. All patients demonstrated cardiac involvement characterized by high-grade AV block at young ages and important right ventricular (RV) involvement. RV predominance was demonstrated by the presence of right bundle branch block in 10 patients (sometimes as a first manifestation) and by RV heart failure in 6 patients, including 2 patients who fulfilled the diagnostic criteria for arrhythmogenic RV cardiomyopathy. Because of this clinical overlap with desmosome cardiomyopathies, we also studied the organization of the intercalated disks, particularly the distribution of desmosomal proteins. Normal amounts of the major desmosomal proteins were found, but the intercalated disks were more convoluted and elongated and had a zigzag appearance.In this largest series to date of individuals with a single head domain DES mutation, patients show a variable yet predominantly cardiologic phenotype characterized by conduction disease at an early age and RV involvement including right bundle branch block and/or RV tachycardias and arrhythmogenic RV cardiomyopathy phenocopies. A localized effect of desmin on the structure of the cardiac intercalated disks might contribute to disease pathogenesis.
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