Clinical, pathological, imaging, and genetic characterization in a Taiwanese cohort with limb-girdle muscular dystrophy
| Autor: | Wan-Zi Chen, Yuh-Jyh Jong, Chien-Hua Wang, Ichizo Nishino, Tzu-Min Kan, Narihiro Minami, Xia Tian, Wen-Chen Liang, Chen-Hua Wang, Lee-Jun C. Wong |
|---|---|
| Jazyk: | angličtina |
| Rok vydání: | 2020 |
| Předmět: |
musculoskeletal diseases
Weakness Pathology medicine.medical_specialty lcsh:Medicine LMNA Cohort Studies Medicine Humans Pharmacology (medical) Genetic Testing Pentosyltransferases Muscular dystrophy Alpha-dystroglycanopathy Genetics (clinical) SGCA Muscle biopsy medicine.diagnostic_test business.industry Genetic heterogeneity Research lcsh:R Facial weakness General Medicine medicine.disease Muscle imaging Phenotype Muscular Dystrophies Limb-Girdle Mutation Next-generation sequencing Limb-girdle muscular dystrophy medicine.symptom business |
| Zdroj: | Orphanet Journal of Rare Diseases, Vol 15, Iss 1, Pp 1-10 (2020) Orphanet Journal of Rare Diseases |
| ISSN: | 1750-1172 |
| DOI: | 10.1186/s13023-020-01445-1 |
| Popis: | Background Limb-girdle muscular dystrophy (LGMD) is a genetically heterogeneous, hereditary disease characterized by limb-girdle weakness and histologically dystrophic changes. The prevalence of each subtype of LGMD varies among different ethnic populations. This study for the first time analyzed the phenotypes and genotypes in Taiwanese patients with LGMD in a referral center for neuromuscular diseases (NMDs). Results We enrolled 102 patients clinically suspected of having LGMD who underwent muscle biopsy with subsequent genetic analysis in the previous 10 years. On the basis of different pathological categories, we performed sequencing of target genes or panel for NMDs and then identified patients with type 1B, 1E, 2A, 2B, 2D, 2I, 2G, 2 N, and 2Q. The 1B patients with LMNA mutation presented with mild limb-girdle weakness but no conduction defect at the time. All 1E patients with DES mutation exhibited predominantly proximal weakness along with distal weakness. In our cohort, 2B and 2I were the most frequent forms of LGMD; several common or founder mutations were identified, including c.1097_1099delACA (p.Asn366del) in DES, homozygous c.101G > T (p.Arg34Leu) in SGCA, homozygous c.26_33dup (p.Glu12Argfs*20) in TCAP, c.545A > G (p.Tyr182Cys), and c.948delC (p.Cys317Alafs*111) in FKRP. Clinically, the prevalence of dilated cardiomyopathy in our patients with LGMD2I aged > 18 years was 100%, much higher than that in European cohorts. The only patient with LGMD2Q with PLEC mutation did not exhibit skin lesions or gastrointestinal abnormalities but had mild facial weakness. Muscle imaging of LGMD1E and 2G revealed a more uniform involvement than did other LGMD types. Conclusion Our study revealed that detailed clinical manifestation together with muscle pathology and imaging remain critical in guiding further molecular analyses and are crucial for establishing genotype–phenotype correlations. We also determined the common mutations and prevalence for different subtypes of LGMD in our cohort, which could be useful when providing specific care and personalized therapy to patients with LGMD. |
| Databáze: | OpenAIRE |
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