Finsterer J
Neurologische Abteilung, KA Rudolfstiftung, Wien, Osterreich.
Nervenarzt. 2004 Dec;75(12):1153-66. doi: 10.1007/s00115-004-1769-5.
Limb girdle muscular dystrophies (LGMDs) are a genetically heterogeneous group of primary myopathies involving progressive weakness and wasting of the muscles in the hip and shoulder girdles, with distal spread to the bulbar or respiratory musculature in rare cases. Depending on the mode of genetic transmission, six autosomal dominant forms (LGMD1A-F, 10-25%) and ten autosomal recessive forms (LGMD2A-J, 75-90%) are currently known. The prevalence of LGMDs is 0.8/100,000. These conditions are caused by mutations in genes encoding for myotilin (5q31, LGMD1A), lamin A/C (1q11-q21.2, LGMD1B), caveolin-3 (3p25, LGMD1C), unknown proteins (7q, LGMD1D, 6q23, LGMD1E, 7q32.1-32.2., LGMD1F), calpain-3 (15q15.1-21.1, LGMD2A), dysferlin (2p13.3-13.1, LGMD2B), gamma-sarcoglycan (13q12, LGMD2C), alpha-sarcoglycan, also known as adhalin (17q12-q21.3, LGMD2D), beta-sarcoglycan (4q12, LGMD2E), delta-sarcoglycan (5q33-q34, LGMD2F), telethonin (17q11-q12, LGMD2G), E3-ubiquitin ligase (9q31-q34.1, LGMD2H), fukutin-related protein (19q13.3, LGMD2I), and titin (2q31, LGMD2J). Cardiac involvement has been described for LGMD1B-E, LGMD2C-G, and LGMD2I. The time of onset varies between early childhood and middle age. There is no male or female preponderance. Disease progression and life expectancy vary widely, even among different members of the same family. The diagnosis is based primarily on DNA analysis. The history, clinical neurological examinations, blood chemistry investigations, electromyography, and muscle biopsy also provide information that is helpful for the diagnosis. No causal therapy is currently available.
肢带型肌营养不良症(LGMDs)是一组遗传性异质性的原发性肌病,其特征为髋部和肩部带肌进行性无力和萎缩,少数情况下可远端累及延髓或呼吸肌。根据遗传传递方式,目前已知有六种常染色体显性形式(LGMD1A - F,占10 - 25%)和十种常染色体隐性形式(LGMD2A - J,占75 - 90%)。LGMDs的患病率为0.8/100,000。这些病症是由编码以下蛋白的基因突变引起的:肌联蛋白(5q31,LGMD1A)、核纤层蛋白A/C(1q11 - q21.2,LGMD1B)、小窝蛋白 - 3(3p25,LGMD1C)、未知蛋白(7q,LGMD1D,6q23,LGMD1E,7q32.1 - 32.2,LGMD1F)、钙蛋白酶 - 3(15q15.1 - 21.1,LGMD2A)、dysferlin(2p13.3 - 13.1,LGMD2B)、γ - 肌聚糖(13q12,LGMD2C)、α - 肌聚糖,也称为粘着蛋白(17q12 - q21.3,LGMD2D)、β - 肌聚糖(4q12,LGMD2E)、δ - 肌聚糖(5q33 - q34,LGMD2F)、肌联蛋白(telethonin)(17q11 - q12,LGMD2G)、E3泛素连接酶(9q31 - q34.1,LGMD2H)、福库汀相关蛋白(19q13.3,LGMD2I)和肌联蛋白(titin)(2q31,LGMD2J)。已报道LGMD1B - E、LGMD2C - G和LGMD2I可累及心脏。发病时间在幼儿期至中年期之间不等。无明显的性别倾向。疾病进展和预期寿命差异很大,即使在同一家族的不同成员之间也是如此。诊断主要基于DNA分析。病史、临床神经学检查、血液化学检查、肌电图和肌肉活检也能提供有助于诊断的信息。目前尚无因果性治疗方法。
