An unusual ryanodine receptor 1 (RYR1) phenotype

Author:

Jokela ManuORCID,Tasca GiorgioORCID,Vihola AnnaORCID,Mercuri EugenioORCID,Jonson Per-HaraldORCID,Lehtinen Sara,Välipakka SallaORCID,Pane Marika,Donati Maria,Johari MridulORCID,Savarese MarcoORCID,Huovinen Sanna,Isohanni Pirjo,Palmio Johanna,Hartikainen Päivi,Udd BjarneORCID

Abstract

ObjectiveTo identify the genetic defect causing a distal calf myopathy with cores.MethodsFamilies with a genetically undetermined calf-predominant myopathy underwent detailed clinical evaluation, including EMG/nerve conduction studies, muscle biopsy, laboratory investigations, and muscle MRI. Next-generation sequencing and targeted Sanger sequencing were used to identify the causative genetic defect in each family.ResultsA novel deletion-insertion mutation in ryanodine receptor 1 (RYR1) was found in the proband of the index family and segregated with the disease in 6 affected relatives. Subsequently, we found 2 more families with a similar calf-predominant myopathy segregating with unique RYR1-mutated alleles. All patients showed a very slowly progressive myopathy without episodes of malignant hyperthermia or rhabdomyolysis. Muscle biopsy showed cores or core-like changes in all families.ConclusionsOur findings expand the spectrum of RYR1-related disorders to include a calf-predominant myopathy with core pathology and autosomal dominant inheritance. Two families had unique and previously unreported RYR1 mutations, while affected persons in the third family carried 2 previously known mutations in the same dominant allele.

Publisher

Ovid Technologies (Wolters Kluwer Health)

Subject

Neurology (clinical)

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