Abstract
Large-scale mitochondrial DNA (mtDNA) deletions are an important cause of mitochondrial disease, while somatic mtDNA deletions cause focal respiratory chain deficiency associated with ageing and neurodegenerative disorders. As mtDNA deletions only cause cellular pathology at high levels of mtDNA heteroplasmy, an mtDNA deletion must accumulate to levels which can result in biochemical dysfunction—a process known as clonal expansion. A number of hypotheses have been proposed for clonal expansion of mtDNA deletions, including a replicative advantage for deleted mitochondrial genomes inferred by their smaller size—implying that the largest mtDNA deletions would also display a replicative advantage over smaller mtDNA deletions. We proposed that in muscle fibres from patients with mtDNA maintenance disorders, which lead to the accumulation of multiple mtDNA deletions, we would observe the largest mtDNA deletions spreading the furthest longitudinally through individual muscle fibres by means of a greater rate of clonal expansion. We characterized mtDNA deletions in patients with mtDNA maintenance disorders from a range of ‘large’ and ‘small’ cytochrome c oxidase (COX)-deficient regions in skeletal muscle fibres. We measured the size of clonally expanded deletions in 62 small and 60 large individual COX-deficient f regions. No significant difference was observed in individual patients or in the total dataset (small fibre regions mean 6.59 kb—large fibre regions mean 6.51 kb). Thus no difference existed in the rate of clonal expansion throughout muscle fibres between mtDNA deletions of different sizes; smaller mitochondrial genomes therefore do not appear to have an inherent replicative advantage in human muscle.
Highlights
Large-scale mitochondrial DNA deletions are an important cause of mitochondrial disease [1]
Longitudinal sections of muscle biopsy underwent histochemical assessment of c oxidase (COX) activity; COX-deficient regions of muscle fibres were targeted for investigation in this study, representing fibre areas where mitochondrial activity has been disrupted to a sufficient degree by mitochondrial DNA (mtDNA) deletion accumulation to cause a biochemical defect
The area of COX-deficiency is a better measure of the spread and accumulation of the mtDNA deletion species responsible for the biochemical defect since measurements based on length fail to take into consideration fibre-width variation
Summary
Large-scale mitochondrial DNA (mtDNA) deletions are an important cause of mitochondrial disease [1]. In many patients these are sporadic single large-scale mtDNA deletions, with the deletion present from birth and the same in all tissues. In patients with mtDNA maintenance disorders the mtDNA deletions found even in adjacent cells is different. This is very similar to the mtDNA deletions which are implicated in the focal cellular dysfunction observed in both ageing and age-related neurodegenerative disease (2 – 5).
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