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首页> 外文期刊>Molecular Genetics and Metabolism Reports >Only some patients with bulbar and spinal muscular atrophy may develop cardiac disease
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Only some patients with bulbar and spinal muscular atrophy may develop cardiac disease

机译:只有一些患有延髓和脊髓性肌萎缩的患者可能会发展为心脏病

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Objectives According to recent publications, some patients with spinal and bulbar muscular atrophy (BSMA) develop cardiac disease, manifesting as ST-segment abnormalities, Brugada-syndrome, dilative cardiomyopathy, or sudden cardiac death. Here we present neurological and cardiac data of a BSMA patient who was followed up for 10 y. Case report In a male patient aged 47 y, BSMA was diagnosed at age 37 y upon the typical clinical presentation (postural tremor since age 12 y, dysarthria since age 15 y, muscle cramps since age 29 y, general myalgias since age 32 y, general fasciculations since age 34 y, myoclonic jerks, easy fatigability, dyspnea upon exercise since age 36 y) and a CAG-repeat expansion of 47 ± 1 repeats in the androgen-receptor gene detected at age 37 y. During the next 10 y he additionally developed mild but slowly progressive diffuse weakness on the upper limbs and mild proximal weakness on the lower limbs. Cardiologic exam, ECG, and echocardiography were normal at ages 37 y, 41 y, 44 y, and 47 y. Conclusions Cardiac involvement may only develop in some BSMA patients within 10 y, whereas neurologic abnormalities slowly progress within 10 y of observation. Cardiac disease may develop at a later stage with progression of age and disease.
机译:目的根据最近的出版物,一些患有脊髓和延髓性肌萎缩症(BSMA)的患者会发展为心脏病,表现为ST段异常,Brugada综合征,扩张型心肌病或心源性猝死。在这里,我们介绍了一名BSMA患者的神经和心脏数据,随访了10年。病例报告在47岁的男性患者中,根据典型的临床表现,BSMA在37岁时被诊断出(自12岁起体位震颤,自15岁起构音困难,自29岁起肌肉痉挛,自32岁起一般肌痛,从34岁开始就表现出一般的束缚,肌阵挛性抽搐,易疲劳,从36岁以后开始运动时呼吸困难)和在37岁时检测到的雄激素受体基因中CAG重复的重复性达到47±1重复。在接下来的10年中,他还在上肢发展出轻度但缓慢进行性弥漫性肌无力,在下肢发展出轻度的近端肌无力。在37岁,41岁,44岁和47岁时,心脏检查,心电图和超声心动图检查正常。结论心脏受累可能仅在某些BSMA患者中在10 y内发展,而神经系统异常在观察到的10 y内缓慢发展。心脏疾病可能随着年龄和疾病的发展而发展。

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