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Null variants in <scp> <i>DYSF</i> </scp> result in earlier symptom onset

Hyung Jun Park, Young Bin Hong, Ji‐Man Hong, UnKyu Yun, Seung Woo Kim, Ha Young Shin, Seung Min Kim, Young‐Chul Choi

2020Clinical Genetics16 citationsDOIOpen Access PDF

Abstract

We investigated the clinical, laboratory, and genetic spectra in Korean patients with dysferlinopathy to clarify its genotype-phenotype correlation. We retrospectively reviewed 101 patients from 96 unrelated families with pathogenic variants of DYSF. The most common initial phenotype was Miyoshi myopathy in 50 patients. Median ages at examination and symptom onset were 23 [interquartile range (IQR): 18-30] and 36 years [IQR: 27-48], respectively. We observed 38 variants, including nine novel variants. Four variants (c.2494C > T, c.1284 + 2 T > C, c.663 + 1G > C, and c.2997G > T) in DYSF accounted for 62% of total allele frequencies of pathogenic variants. To analyze the genotype-phenotype correlation, we compared the clinical phenotype between patients with null/null (N/N; n = 55) and null/missense variants (N/M; n = 35). The N/N group had an earlier symptom onset age (median: 20 years [IQR: 17-25]) than the N/M group (median: 29 years [IQR: 23-35], p < .001). Total manual muscle testing scores in lower extremities were lower in the N/N group (median: 80 [IQR: 56-92]) than in the N/M group (median: 89 [IQR: 78-98], p = .013). Our study is the first to report that null variants in DYSF result in an earlier symptom onset than missense variants.

Topics & Concepts

Interquartile rangeMissense mutationGastroenterologyMedicineGenotypePhenotypeInternal medicineAlleleNull alleleGeneticsBiologyGeneMuscle Physiology and DisordersGenetic Syndromes and ImprintingNeurogenetic and Muscular Disorders Research
Null variants in <scp> <i>DYSF</i> </scp> result in earlier symptom onset | Litcius