Rapid Molecular Diagnosis of Genetically Inherited Neuromuscular Disorders Using Next-Generation Sequencing Technologies

Overview

Journal J Clin Med

Specialty General Medicine

Date 2022 May 28

PMID 35628876

Authors

Sofia Barbosa-Gouveia

Maria Eugenia Vazquez-Mosquera

Emiliano Gonzalez-Vioque

Alvaro Hermida-Ameijeiras

Paula Sanchez-Pintos

Maria Jose de Castro

Soraya Ramiro Leon

Belen Gil-Fournier

Cristina Dominguez-Gonzalez

Ana Camacho Salas

Luis Negrao

Isabel Fineza

Francisco Laranjeira

Maria Luz Couce

Affiliations

Soon will be listed here.

Abstract

Neuromuscular diseases are genetically highly heterogeneous, and differential diagnosis can be challenging. Over a 3-year period, we prospectively analyzed 268 pediatric and adult patients with a suspected diagnosis of inherited neuromuscular disorder (INMD) using comprehensive gene-panel analysis and next-generation sequencing. The rate of diagnosis increased exponentially with the addition of genes to successive versions of the INMD panel, from 31% for the first iteration (278 genes) to 40% for the last (324 genes). The global mean diagnostic rate was 36% (97/268 patients), with a diagnostic turnaround time of 4-6 weeks. Most diagnoses corresponded to muscular dystrophies/myopathies (68.37%) and peripheral nerve diseases (22.45%). The most common causative genes, , , and , accounted for almost 30% of the diagnosed cases. Finally, we evaluated the utility of the differential diagnosis tool Phenomizer, which established a correlation between the phenotype and molecular findings in 21% of the diagnosed patients. In summary, comprehensive gene-panel analysis of all genes implicated in neuromuscular diseases facilitates a rapid diagnosis and provides a high diagnostic yield.

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