Abstract

Distal myopathies are genetically heterogeneous. TIA1 mutations cause Welander distal myopathy. MYH7 mutations result in various clinical phenotypes, including Laing distal myopathy, myosin storage myopathy and hypertrophic/dilated cardiomyopathy. We describe a family affected by distal myopathy and variable presence of cardiomyopathy due to coexisting TIA1 and MYH7 mutations. The propositus is a 67-year-old woman of Swedish and Greek descent with history of easy tripping since childhood who has experienced a stepwise progression of asymmetric distal limb weakness in the past 20 years. Neurological examination revealed mild to severe asymmetric distal lower >upper limb weakness. CK value was normal. EMG study showed myopathic changes with minimal fibrillation potentials and myotonic discharges. Biopsy of the extensor carpi radialis muscle showed: rare rimmed vacuoles, minicore-like structures and congophilic inclusions; few necrotic and regenerating fibers; fiber splitting; increased internal nuclei; and fiber type grouping. There was no cardiac involvement by ECG and echocardiogram. Her 66-year-old sister has 8 years of mild distal limb weakness, supraventricular tachycardia and hypertrophic cardiomyopathy documented by echocardiogram and MRI. Another sibling has distal weakness while parents were asymptomatic. Both sisters carry a known pathogenic heterozygous TIA1 mutation (p.Glu384Lys) and a rare heterozygous MYH7 variant (c.5459G > A; p.Arg1820Gln), which involves a highly conserved residue and is predicted to be pathogenic. Because a homozygous MYH7 mutation (p.Arg1820Trp) was reported in recessive myosin storage myopathy, aCGH deletion/duplication analysis of MYH7 was performed in the proband and it was normal. The clinical phenotype is dictated by the coexistent TIA1 and MYH7 mutations, which can result in similar pathological findings. The proband's early onset of distal leg weakness and the sister's cardiomyopathy support the pathogenicity of the MYH7.

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