Interpreting the clinical significance of multiple large-scale mitochondrial DNA deletions (MLSMD) in skeletal muscle tissue in the diagnostic evaluation of primary mitochondrial disease
Jing Wang, James T. Peterson, Joaquim Diego D. Santos, Ada J. S. Chan, Maria Alejandra Diaz-Miranda, Imon Rahaman, Jean Flickinger, Amy Goldstein, Emily Bogush, Elizabeth M. McCormick, Colleen C. Muraresku, Vernon E. Anderson, Matthew C. Dulik, Douglas C. Wallace, Rui Xiao

TL;DR
This study examines the clinical significance of multiple large-scale mitochondrial DNA deletions in muscle tissue and their association with mitochondrial disease.
Contribution
The study identifies a promising cohort for novel gene discoveries in mitochondrial disease.
Findings
MLSMD were found in 24% of diagnostic muscle biopsies and were universally present in subjects over 50 years.
Subjects with MLSMD showed more mitochondrial abnormalities and enzyme upregulation compared to those without MLSMD.
A subset of MLSMD patients with suspected PMD showed more biochemical and histopathological abnormalities.
Abstract
Improved detection sensitivity from combined Long-Range PCR (LR-PCR), Next-Generation Sequencing (NGS), and droplet digital PCR (ddPCR) to identify multiple large-scale mtDNA deletions (MLSMD) and quantify deletion heteroplasmy have introduced clinical interpretation challenges. We sought to evaluate clinical, biochemical, and histopathological phenotypes of a large clinical cohort harboring MLSMD in muscle to better understand their significance across a range of clinical phenotypes. A single-site retrospective study was performed of 212 diagnostic muscle biopsies obtained from patients referred for Primary Mitochondrial Disease (PMD) evaluation with muscle mitochondrial (mt)DNA sequencing performed at our institution, including electronic medical record (EMR) review of symptoms, biochemical results, and Mitochondrial Myopathy Composite Assessment Tool (MM-COAST) scores. MLSMD were…
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Taxonomy
TopicsMitochondrial Function and Pathology · Metabolism and Genetic Disorders · Genetic Neurodegenerative Diseases
