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. 2020 Jan 29;20(1):41.
doi: 10.1186/s12887-020-1912-x.

Multisystem mitochondrial diseases due to mutations in mtDNA-encoded subunits of complex I

Tereza Danhelovska  1 Hana Kolarova  1 Jiri Zeman  1 Hana Hansikova  1 Manuela Vaneckova  2 Lukas Lambert  2 Vendula Kucerova-Vidrova  1 Kamila Berankova  1 Tomas Honzik  1 Marketa Tesarova  3
Affiliations

Multisystem mitochondrial diseases due to mutations in mtDNA-encoded subunits of complex I

Tereza Danhelovska et al. BMC Pediatr. .

Abstract

Background: Maternally inherited complex I deficiencies due to mutations in MT-ND genes represent a heterogeneous group of multisystem mitochondrial disorders (MD) with a unfavourable prognosis. The aim of the study was to characterize the impact of the mutations in MT-ND genes, including the novel m.13091 T > C variant, on the course of the disease, and to analyse the activities of respiratory chain complexes, the amount of protein subunits, and the mitochondrial energy-generating system (MEGS) in available muscle biopsies and cultivated fibroblasts.

Methods: The respiratory chain complex activities were measured by spectrophotometry, MEGS were analysed using radiolabelled substrates, and protein amount by SDS-PAGE or BN-PAGE in muscle or fibroblasts.

Results: In our cohort of 106 unrelated families carrying different mtDNA mutations, we found heteroplasmic mutations in the genes MT-ND1, MT-ND3, and MT-ND5, including the novel variant m.13091 T > C, in 13 patients with MD from 12 families. First symptoms developed between early childhood and adolescence and progressed to multisystem disease with a phenotype of Leigh or MELAS syndromes. MRI revealed bilateral symmetrical involvement of deep grey matter typical of Leigh syndrome in 6 children, cortical/white matter stroke-like lesions suggesting MELAS syndrome in 3 patients, and a combination of cortico-subcortical lesions and grey matter involvement in 4 patients. MEGS indicated mitochondrial disturbances in all available muscle samples, as well as a significantly decreased oxidation of [1-14C] pyruvate in fibroblasts. Spectrophotometric analyses revealed a low activity of complex I and/or complex I + III in all muscle samples except one, but the activities in fibroblasts were mostly normal. No correlation was found between complex I activities and mtDNA mutation load, but higher levels of heteroplasmy were generally found in more severely affected patients.

Conclusions: Maternally inherited complex I deficiencies were found in 11% of families with mitochondrial diseases in our region. Six patients manifested with Leigh, three with MELAS. The remaining four patients presented with an overlap between these two syndromes. MEGS, especially the oxidation of [1-14C] pyruvate in fibroblasts might serve as a sensitive indicator of functional impairment due to MT-ND mutations. Early onset of the disease and higher level of mtDNA heteroplasmy were associated with a worse prognosis.

Keywords: Complex I; Leigh syndrome; MEGS; MELAS syndrome; MT-ND genes; Mitochondria; mtDNA.

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Conflict of interest statement

The authors declare that they have no competing interests.

Figures

Fig. 1
Fig. 1
MRI of the brain in P1–P3 and P5–P12 with complex I deficiency. Signal changes in basal ganglia or brainstem characteristic for Leigh syndrome are present in patients P2, P6, P9, P10 and P13. Signal changes in the cortex and white matter of the hemispheres or cerebellum with stroke-like lesion are present in patients P5, P8, P11, and the combination of both changes are visible in patients P1, P3, P7 and P12. Moderate to severe periventricular atrophy was found in patients P1, P3 and P5.
Fig. 2
Fig. 2
Protein analysis in six patients with heteroplasmic mutations in MT-ND5 gene. a Comparison of steady-state levels of several OXPHOS-related proteins in P5, P6, P7, P9 and P10 in fibroblasts using SDS-PAGE/WB. As a control was used primary dermal fibroblasts (ATCC® PCS-201-010™), 50 and 100% demonstrate loading dose of protein amount. b BN-PAGE/WB of OXPHOS complexes in isolated mitochondria from the muscle of P8. As a control was used human muscle mitochondria from heathy adult, 25; 50 and 100% demonstrate loading dose of protein amount. c The quantification of western blot signals from A by densitometric analysis. Relative signals intensity of individual OXPHOS antibodies were normalized to intensity of loading control β-tubulin. d The quantification of western blot signals from B by densitometric analysis
Fig. 3
Fig. 3
Oxidation rate of 4 different MEGS incubations containing [1-14C] pyruvate in cultivated skin fibroblasts. Patient group consists of 8 patients (P1, P2, P4, P6, P7, and P9–P11) with complex I deficiency and heteroplasmic mutations in MT-ND1, MT-ND3 and MT-ND5 genes. Control group consists of 10 age-related controls. In the group of patients, oxidation rate of all four displayed MEGS incubations are significantly decreased (*p < 0.05). Open circles displayed suspected outliers
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