MtDNA Heteroplasmy Level and Copy Number Indicate Disease Burden in M.3243A>G Mitochondrial Disease

Overview

Journal EMBO Mol Med

Specialty Molecular Biology

Date 2018 May 9

PMID 29735722

Citations 121

Authors

John P Grady

Sarah J Pickett

Yi Shiau Ng

Charlotte L Alston

Emma L Blakely

Steven A Hardy

Catherine L Feeney

Alexandra A Bright

Andrew M Schaefer

Grainne S Gorman

Richard Jq McNally

Robert W Taylor

Doug M Turnbull

Robert McFarland

Affiliations

Soon will be listed here.

Abstract

Mitochondrial disease associated with the pathogenic m.3243A>G variant is a common, clinically heterogeneous, neurogenetic disorder. Using multiple linear regression and linear mixed modelling, we evaluated which commonly assayed tissue (blood = 231, urine = 235, skeletal muscle = 77) represents the m.3243A>G mutation load and mitochondrial DNA (mtDNA) copy number most strongly associated with disease burden and progression. m.3243A>G levels are correlated in blood, muscle and urine ( = 0.61-0.73). Blood heteroplasmy declines by ~2.3%/year; we have extended previously published methodology to adjust for age. In urine, males have higher mtDNA copy number and ~20% higher m.3243A>G mutation load; we present formulas to adjust for this. Blood is the most highly correlated mutation measure for disease burden and progression in m.3243A>G-harbouring individuals; increasing age and heteroplasmy contribute ( = 0.27, < 0.001). In muscle, heteroplasmy, age and mtDNA copy number explain a higher proportion of variability in disease burden ( = 0.40, < 0.001), although activity level and disease severity are likely to affect copy number. Whilst our data indicate that age-corrected blood m.3243A>G heteroplasmy is the most convenient and reliable measure for routine clinical assessment, additional factors such as mtDNA copy number may also influence disease severity.

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