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瞬间酿成的悲剧:结蛋白功能异常引发骨骼肌和心肌疾病。

Tragedy in a heartbeat: malfunctioning desmin causes skeletal and cardiac muscle disease.

作者信息

Goldfarb Lev G, Dalakas Marinos C

机构信息

National Institute of Neurological Disorders and Stroke, NIH, Bethesda, MD 20892, USA.

出版信息

J Clin Invest. 2009 Jul;119(7):1806-13. doi: 10.1172/JCI38027. Epub 2009 Jul 1.

Abstract

Muscle fiber deterioration resulting in progressive skeletal muscle weakness, heart failure, and respiratory distress occurs in more than 20 inherited myopathies. As discussed in this Review, one of the newly identified myopathies is desminopathy, a disease caused by dysfunctional mutations in desmin, a type III intermediate filament protein, or alphaB-crystallin, a chaperone for desmin. The range of clinical manifestations in patients with desminopathy is wide and may overlap with those observed in individuals with other myopathies. Awareness of this disease needs to be heightened, diagnostic criteria reliably outlined, and molecular testing readily available; this would ensure prevention of sudden death from cardiac arrhythmias and other complications.

摘要

20多种遗传性肌病会出现肌肉纤维退化,导致进行性骨骼肌无力、心力衰竭和呼吸窘迫。如本综述所述,新发现的肌病之一是结蛋白病,该病由III型中间丝蛋白结蛋白或结蛋白伴侣αB晶状体蛋白的功能异常突变引起。结蛋白病患者的临床表现范围广泛,可能与其他肌病患者的表现重叠。需要提高对这种疾病的认识,可靠地概述诊断标准,并提供便捷的分子检测;这将确保预防心律失常和其他并发症导致的猝死。

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