Late-onset myopathy of the posterior calf muscles mimicking Miyoshi myopathy unrelated to dysferlin mutation: A case report

被引：6

作者：

Clemens Neusch

Tanja Kuhlmann

Wolfram Kress

Christiane Schneider-Gold

机构：

[1] Department of Neurology, University of Ulm, Ulm

[2] Institute of Neuropathology, University Hospital Münster, Münster

[3] Institute of Human Genetics, University of Würzburg, Biozentrum, Würzburg, 97074, Am Hubland

[4] Department of Neurology, University of Bochum, St Josef Hospital, Bochum

来源：

Journal of Medical Case Reports | / 6卷 / 1期

关键词：

Myopathy; Gastrocnemius Muscle; Calf Muscle; Compound Muscle Action Potential Amplitude; Distal Myopathy;

D O I：

10.1186/1752-1947-6-345

中图分类号：

学科分类号：

摘要：

Introduction. Miyoshi myopathy, a type of distal myopathy with predominant involvement of the posterior calf muscles, has been assigned to mutations in the dysferlin gene. However, many of the late-onset limb-girdle and distal myopathies that resemble dysferlinopathy or Miyoshi myopathy remain unclassified, even after extensive immunohistological and genetic analysis. Case presentation. We report the case of a 59-year-old Caucasian man with distal myopathy and exercise-induced myalgia, preferentially of the leg muscles, closely resembling the Miyoshi phenotype. Magnetic resonance imaging of his calf muscles showed typical fatty replacement of the medial heads of the gastrocnemius muscles and soleus muscles, with progression to the adductor longus muscles over a time course of two years. However, genetic analysis revealed that the phenotype of our patient was not related to a mutation in the dysferlin gene but to a novel homozygous splice mutation in the anoctamin 5 gene. Mutations in the anoctamin 5 gene have so far been identified only in some cases of limb-girdle and distal myopathy. Mutations in the anoctamin 5 gene have been assigned to limb-girdle muscular dystrophy type 2L, while distal Miyoshi-like phenotypes have been classified as Miyoshi myopathy type 3. Conclusion: The case presented in this report further strengthens the underlying genetic heterogeneity in Miyoshi myopathy-like phenotypes and adds another family to non-dysferlin, Miyoshi myopathy type 3 of late-onset. Furthermore, our case supports the recent observation that anoctamin 5 mutations are a primary cause of distal non-dysferlin myopathies. Therefore, given the increasing number of anoctamin 5 mutations in Miyoshi-like phenotypes, genetic analysis should include an anoctamin 5 screen in late-onset limb-girdle and distal myopathies. © 2012 Neusch et al.; licensee BioMed Central Ltd.

引用

共 10 条

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