Selcen Duygu, Ohno Kinji, Engel Andrew G
Department of Neurology, Neuromuscular Research Laboratory, Mayo Clinic, 200 First Street SW, Rochester, MN 55905, USA.
Brain. 2004 Feb;127(Pt 2):439-51. doi: 10.1093/brain/awh052. Epub 2004 Jan 7.
The term myofibrillar myopathy (MFM) was proposed in 1996 as a non-committal term for a pathological pattern of myofibrillar dissolution associated with accumulation of myofibrillar degradation products and ectopic expression of multiple proteins that include desmin, alphaB-crystallin (alphaBC), dystrophin and congophilic amyloid material. Subsequent studies revealed dominant mutations in desmin and alphaBC in some MFM patients, and clinical differences between kinships. We here review the clinical, structural and genetic features of 63 unrelated patients diagnosed as having MFM at the Mayo Clinic between 1977 and 2003. The age of onset was 54 +/- 16 years (mean +/- SD). Weakness was both proximal and distal in 77% and proximal only in 13%. Cardiomyopathy was diagnosed in 16%. Electro myography revealed a myopathic pattern associated with abnormal electrical irritability; 13 patients had abnormal nerve conduction studies but four of these had long-standing diabetes. The abnormal muscle fibres are best identified in trichrome-stained sections as harbouring amorphous, granular or pleomorphic hyaline structures, and vacuoles containing membranous material. The hyaline structures are strongly congophilic. Semiquantitative analysis in each case indicates that among the abnormal fibres, an average of 90, 75, 75, 70 and 70% abnormally express myotilin, desmin, alphaBC, dystrophin and beta-amyloid precursor protein, respectively. Therefore, immunostains for these proteins, and especially for myotilin, are useful adjuncts in the diagnosis of MFM. Electron microscopy shows progressive myofibrillar degeneration commencing at the Z-disk, accumulation of degraded filamentous material and entrapment of dislocated membranous organelles in autophagic vacuoles. In all patients, we searched for mutations in desmin and alphaBC, as well as in telethonin, a Z-disk-associated protein, or in syncoilin, which together with plectin links desmin to the Z-disk. Two of the 63 patients carry truncation mutations in the C-terminal domain of alphaBC, four carry missense mutations in the head or tail region of desmin, and none carries a mutation in syncoilin or telethonin. Thus, MFM is morphologically distinct but genetically heterogeneous. Further advances in defining the molecular causes of MFM will probably come from linkage studies of informative kinships or from systematic search for mutations in proteins participating in the intricate network supporting the Z-disk.
肌原纤维肌病(MFM)这一术语于1996年被提出,作为一个不明确的术语,用于描述一种肌原纤维溶解的病理模式,该模式与肌原纤维降解产物的积累以及多种蛋白质的异位表达相关,这些蛋白质包括结蛋白、αB-晶状体蛋白(αBC)、肌营养不良蛋白和嗜刚果红淀粉样物质。随后的研究揭示了一些MFM患者中结蛋白和αBC的显性突变,以及家族之间的临床差异。我们在此回顾了1977年至2003年间在梅奥诊所被诊断为患有MFM的63例无亲缘关系患者的临床、结构和遗传特征。发病年龄为54±16岁(平均值±标准差)。77%的患者近端和远端均有肌无力,13%的患者仅近端有肌无力。16%的患者被诊断患有心肌病。肌电图显示为与异常电兴奋性相关的肌病模式;13例患者神经传导研究异常,但其中4例患有长期糖尿病。在三色染色切片中,异常肌纤维最易被识别为含有无定形、颗粒状或多形性透明结构,以及含有膜性物质的空泡。这些透明结构强烈嗜刚果红。每例病例的半定量分析表明,在异常纤维中,平均分别有90%、75%、75%、70%和70%异常表达肌联蛋白、结蛋白、αBC、肌营养不良蛋白和β-淀粉样前体蛋白。因此,这些蛋白质的免疫染色,尤其是肌联蛋白的免疫染色,在MFM的诊断中是有用的辅助手段。电子显微镜显示肌原纤维从Z线开始进行性变性,降解的丝状物质积累,以及自噬泡中错位的膜性细胞器被困。在所有患者中,我们搜索了结蛋白、αBC以及与Z线相关的蛋白隐钙蛋白或与网蛋白一起将结蛋白连接到Z线的伴肌动蛋白的突变。63例患者中有2例在αBC的C末端结构域携带截短突变,4例在结蛋白的头部或尾部区域携带错义突变,而在伴肌动蛋白或隐钙蛋白中均未发现突变。因此,MFM在形态上有明显特征,但在遗传上具有异质性。在确定MFM分子病因方面的进一步进展可能来自对有信息价值的家族进行连锁研究,或来自对参与支持Z线的复杂网络的蛋白质进行系统的突变搜索。
