肌球蛋白重链IIa基因突变E706K具有致病性，且其表达随年龄增长而增加。

Myosin heavy chain IIa gene mutation E706K is pathogenic and its expression increases with age.

作者信息

Tajsharghi H, Thornell L-E, Darin N, Martinsson T, Kyllerman M, Wahlström J, Oldfors A

机构信息

Department of Pathology, Sahlgrenska University Hospital, Gothenburg, Sweden.

出版信息

Neurology. 2002 Mar 12;58(5):780-6. doi: 10.1212/wnl.58.5.780.

DOI:10.1212/wnl.58.5.780

PMID:11889243

Abstract

BACKGROUND

The authors recently described a new autosomal dominant myopathy (OMIM 605637 inclusion body myopathy 3) associated with a missense mutation in the myosin heavy chain (MyHC) IIa gene (MyHC IIa, Human Gene Map [HGM] locus MYH2). Young patients showed minor changes in their muscle biopsies, although dystrophic alterations and rimmed vacuoles with 15- to 20-nm tubulofilaments identical to those in sporadic inclusion body myositis (s-IBM) were observed in some of the adult (especially older) patients. The current study was undertaken to investigate the relation between expression of the mutant MyHC IIa and pathologic changes in muscle.

METHODS

The expression of MyHC IIa in nine muscle specimens from six individuals carrying the mutation was analyzed by immunohistochemistry, sodium dodecyl sulfate-polyacrylamide gel electrophoresis, and a new reverse transcriptase--PCR method to measure the relative abundance of the various MyHC transcripts.

RESULTS

Young patients with muscle weakness and minor pathologic changes in muscle expressed MyHC IIa at undetectable levels. MyHC IIa was expressed at high levels in adults with a progressive clinical course and dystrophic muscle changes. In these cases, a large number of muscle fibers were hybrids with expression of more than one MyHC isoform. Both MyHC IIa alleles were equally expressed. The relative level of MyHC IIa transcripts exceeded that of the corresponding protein, indicating an increased turnover of mutated protein. MyHC IIa expression was a consistent finding in muscle fibers with rimmed vacuoles.

CONCLUSIONS

The clear correlation between pathologic changes and expression of MyHC IIa indicates that defects in MyHC may lead not only to muscle weakness but also to muscle degeneration. The consistent expression of MyHC IIa in muscle fibers with rimmed vacuoles indicates that the breakdown of sarcomeric proteins is a key element in the pathogenesis of rimmed vacuoles of s-IBM type.

摘要

背景

作者最近描述了一种新的常染色体显性遗传肌病（OMIM 605637，包涵体肌病3型），其与肌球蛋白重链（MyHC）IIa基因（MyHC IIa，人类基因图谱[HGM]位点MYH2）中的错义突变相关。年轻患者的肌肉活检显示轻微变化，尽管在一些成年（尤其是老年）患者中观察到营养不良性改变以及与散发性包涵体肌炎（s-IBM）中相同的、含有15至20纳米微管丝的镶边空泡。当前研究旨在调查突变型MyHC IIa的表达与肌肉病理变化之间的关系。

方法

通过免疫组织化学、十二烷基硫酸钠 - 聚丙烯酰胺凝胶电泳以及一种新的逆转录 - PCR方法，分析了来自6名携带该突变个体的9份肌肉标本中MyHC IIa的表达，以测量各种MyHC转录本的相对丰度。

结果

肌肉无力且肌肉病理变化轻微的年轻患者中，MyHC IIa表达水平无法检测到。MyHC IIa在临床病程呈进行性且有营养不良性肌肉变化的成年人中高水平表达。在这些病例中，大量肌纤维是表达不止一种MyHC同工型的杂种。两个MyHC IIa等位基因均等量表达。MyHC IIa转录本的相对水平超过了相应蛋白质的水平，表明突变蛋白的周转增加。MyHC IIa表达在有镶边空泡的肌纤维中是一个一致的发现。