Stem cell modeling of mitochondrial parkinsonism reveals key functions of OPA1

被引:21
作者
Jonikas, Mindaugas [1 ]
Madill, Martin [1 ]
Mathy, Alexandre [1 ]
Zekoll, Theresa [1 ]
Zois, Christos E. [2 ]
Wigfield, Simon [2 ]
Kurzawa-Akanbi, Marzena [3 ]
Browne, Cathy [4 ]
Sims, David [5 ]
Chinnery, Patrick F. [6 ,7 ]
Cowley, Sally A. [4 ]
Tofaris, George K. [1 ]
机构
[1] Univ Oxford, Nuffield Dept Clin Neurosci, Oxford OX3 9DU, England
[2] Univ Oxford, Weatherall Inst Mol Med, Dept Oncol, Oxford, England
[3] Newcastle Univ, Mitochondrial Res Grp, Newcastle Upon Tyne, Tyne & Wear, England
[4] Univ Oxford, Sir William Dunn Sch Pathol, James Martin Stem Cell Facil, Oxford, England
[5] Univ Oxford, MRC Weatherall Inst Mol Med, MRC WIMM Ctr Computat Biol, MRC Computat Genom Anal & Training Programme, Oxford, England
[6] Univ Cambridge, Dept Clin Neurosci, Cambridge, England
[7] MRC Mitochondrial Biol Unit, Cambridge Biomed Campus, Cambridge, England
来源
ANNALS OF NEUROLOGY | 2018年 / 83卷 / 05期
基金
英国惠康基金; 英国医学研究理事会;
关键词
DOMINANT OPTIC ATROPHY; OXIDATIVE-PHOSPHORYLATION; MUTATIONS; FUSION; NEURONS; OMA1; PLURIPOTENCY; MAINTENANCE; APOPTOSIS; DEMENTIA;
D O I
10.1002/ana.25221
中图分类号
R74 [神经病学与精神病学];
学科分类号
摘要
ObjectiveDefective mitochondrial function attributed to optic atrophy 1 (OPA1) mutations causes primarily optic atrophy and, less commonly, neurodegenerative syndromes. The pathomechanism by which OPA1 mutations trigger diffuse loss of neurons in some, but not all, patients is unknown. Here, we used a tractable induced pluripotent stem cell (iPSC)-based model to capture the biology of OPA1 haploinsufficiency in cases presenting with classic eye disease versus syndromic parkinsonism. MethodsiPSCs were generated from 2 patients with OPA1 haploinsufficiency and 2 controls and differentiated into dopaminergic neurons. Metabolic profile was determined by extracellular flux analysis, respiratory complex levels using immunoblotting, and complex I activity by a colorimetric assay. Mitochondria were examined by transmission electron microscopy. Mitochondrial DNA copy number and deletions were assayed using long-range PCR. Mitochondrial membrane potential was measured by tetramethylrhodamine methyl ester uptake, and mitochondrial fragmentation was assessed by confocal microscopy. Exome sequencing was used to screen for pathogenic variants. ResultsOPA1 haploinsufficient iPSCs differentiated into dopaminergic neurons and exhibited marked reduction in OPA1 protein levels. Loss of OPA1 caused a late defect in oxidative phosphorylation, reduced complex I levels, and activity without a significant change in the ultrastructure of mitochondria. Loss of neurons in culture recapitulated dopaminergic degeneration in syndromic disease and correlated with mitochondrial fragmentation. InterpretationOPA1 levels maintain oxidative phosphorylation in iPSC-derived neurons, at least in part, by regulating the stability of complex I. Severity of OPA1 disease associates primarily with the extent of OPA1-mediated fusion, suggesting that activation of this mechanism or identification of its genetic modifiers may have therapeutic or prognostic value. Ann Neurol 2018;83:915-925
引用
收藏
页码:915 / 925
页数:11
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