Core myopathy in two siblings with a biallelic variant in the CACNA1S gene—A case series study-Reference-Cited by-同舟云学术

Core myopathy in two siblings with a biallelic variant in the CACNA1S gene—A case series study

Published:2024-08 Issue:8 Volume:12 Page:
ISSN:2050-0904
Container-title:Clinical Case Reports
language:en
Short-container-title:Clinical Case Reports

Author:

Khoeini Tara¹,Kariminejad Ariana²^ORCID,Nilipour Yalda³⁴,Ariaei Armin⁵^ORCID,Najmabadi Hossein²⁶^ORCID,Arabshahi Mojtaba⁷,Faraji Zonooz Mehrshid²,Haghi Ashtiani Bahram¹

Affiliation:

1. Department of Neurology, Firoozgar Hospital Iran University of Medical Sciences Tehran Iran

2. Kariminejad‐Najmabadi Pathology & Genetics Center Tehran Iran

3. Pediatric Pathology Research Center Research Institute for Children's Health, Shahid Beheshti University of Medical Sciences Tehran Iran

4. Neuromuscular Research Center Tehran University of Medical Sciences Tehran Iran

5. School of Medicine Iran University of Medical Sciences Tehran Iran

6. Genetics Research Center University of Social Welfare & Rehabilitation Science Tehran Iran

7. Radiology Department, Shohada Tajrish Hospital Shahid Beheshti University of Medical Science Tehran Iran

Abstract

Key Clinical MessageHomozygous variants of Calcium Voltage‐Gated Channel Subunit Alpha1 S (CACNA1S) gene mutation were previously identified as causes of periodic paralysis and congenital early‐onset myopathy, while it could be manifested as a late‐onset congenital core myopathy.AbstractCalcium Voltage‐Gated Channel Subunit Alpha1 S (CACNA1S) gene mutation has been linked to various neuromuscular conditions in recent years. Congenital myopathy with core‐like features is one of the cardinal associations reported previously, causing severe respiratory insufficiency and death in neonates. Informed consent was received from the patients. Subsequently, peripheral blood leukocytes were utilized to extract genomic DNA. Moreover, exome enrichment was implemented through the Twist Human Core Exome Kit (Twist Bioscience) and exome sequenced using Illumina NovaSeq 6000 platform (Illumina, San Diego, CA, USA). Sanger sequencing using BIG Dye Terminators confirmed the presence of the final variant. Finally, the candidate variants were classified based on the American College of Medical Genetics and Genomics (ACMG) guidelines. In this report, we describe two siblings, who presented with childhood and late‐onset progressive muscle weakness, and had a homozygous variant in exon 2 of the CACNA1S gene defined as c.188C > A (p.Ala63Asp) (NM_000069.3). The SIFT, Polyphen2, CADD PHRED, and Mutation Taster analysis tools classified the variant as pathogenic/damaging. The muscle biopsy of the younger brother revealed intermyofibrillar network pattern disruption as cytoplasmic core‐like lesions. The muscle magnetic resonance imaging (MRI) reported grade IIa and IIb fatty changes. Finally, the electromyography (EMG) findings suggested a myopathic change pattern. This report illustrates the clinical variability in CACNA1S‐related myopathy by reviewing prior reports and adding newly found aspects, additionally expanding the gene defects associated with core myopathy.

Publisher

Wiley

Link

https://onlinelibrary.wiley.com/doi/pdf/10.1002/ccr3.9251

Reference17 articles.

1. Approach to the diagnosis of congenital myopathies

2. Triadopathies: An Emerging Class of Skeletal Muscle Diseases

3. PharmGKB summary: very important pharmacogene information for CACNA1S

4. Recent Advances and Future Directions in Imaging of Peripheral Nervous System: A Comprehensive Review for Therapeutics Approach

5. Clinical and imaging findings in six cases of congenital muscular dystrophy with rigid spine syndrome linked to chromosome 1p (RSMD1)