Oxidative switch drives mitophagy defects in dopaminergic<i>parkin</i>mutant patient neurons

Schwartzentruber, Aurelie; Boschian, Camilla; Lopes, Fernanda Machado; Myszczynska, Monika A.; New, Elizabeth J.; Smeitink, Jan A.M.; Ferraiuolo, Laura; Mortiboys, Heather

doi:10.1101/2020.05.29.115782

2020

DOI: 10.1101/2020.05.29.115782

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Oxidative switch drives mitophagy defects in dopaminergicparkinmutant patient neurons

Aurelie Schwartzentruber

Camilla Boschian

Fernanda Machado Lopes

et al.

Abstract: 22Background Mutations in parkin are the most common cause of early onset Parkinson's disease. Parkin 23 is an E3 ubiquitin ligase, functioning in mitophagy. Mitochondrial abnormalities are present in parkin 24 mutant models. Patient derived neurons are a promising model in which to study pathogenic 25 mechanisms and therapeutic targets. Here we generate induced neuronal progenitor cells from parkin 26 mutant patient fibroblasts with a high dopaminergic neuron yield. We reveal changing mitochondrial 27 phenoty… Show more

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Deficits in mitochondrial function and glucose metabolism seen in sporadic and familial Alzheimer’s disease derived Astrocytes are ameliorated by increasing hexokinase 1 expression

Bell

Wareing

Hamshaw

et al. 2023

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Background: Astrocytes have multiple roles including providing neurons with metabolic substrates and maintaining neurotransmitter synaptic homeostasis. Astrocyte glucose metabolism plays a key role in learning and memory with astrocytic glycogen a key substrate supporting memory encoding. The neuronal support provided by astrocytes has a high metabolic demand. Deficits in astrocytic mitochondrial metabolic functioning and glycolysis could impair neuronal function. Changes to cellular metabolism are seen early in Alzheimers disease (AD). Understanding cellular metabolism changes in AD astrocytes could be exploited as a new biomarker or synergistic therapeutic agent when combined with anti-amyloid treatments in AD. Methods: In this project, we characterised mitochondrial and glycolytic function in astrocytes derived from patients with sporadic (n=6) and familial (PSEN1, n=3) forms of AD. Astrocytes were derived using direct reprogramming methods. Astrocyte metabolic outputs: ATP, and extracellular lactate levels were measured using luminescent and fluorescent protocols. Mitochondrial respiration and glycolytic function were measured using a Seahorse XF Analyzer. Hexokinase deficits identified where corrected by transfecting astrocytes with an adenovirus viral vector containing the hexokinase 1 gene. Results: There was a reduction of total cellular ATP of 20% (p=0.05 in sAD astrocytes) and of 48% (p<0.01) in fAD. A 44% reduction (p<0.05), and 80% reduction in mitochondrial spare capacity was seen in sAD and fAD astrocytes respectively. Reactive oxygen species (ROS) were increased in both AD astrocyte types (p=0.05). Mitochondrial complex I and II was significantly increased in sAD (p<0.05) but not in fAD. Astrocyte glycolytic reserve and extracellular lactate was significantly reduced when compared to controls in both sAD and fAD (p<0.05). We identified a deficit in the glycolytic pathway enzyme hexokinase, and correcting this deficit restored most of the metabolic phenotype in sAD but not fAD astrocytes. Conclusion: AD astrocytes have abnormalities in functional capacity of mitochondria and the process of glycolysis. These functional deficits can be improved by correcting hexokinase expression deficits with adenoviral vectors. This suggests that hexokinase 1 deficiency could potentially be exploited as a new therapeutic target for AD.

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Deficits in mitochondrial function and glucose metabolism seen in sporadic and familial Alzheimer’s disease derived Astrocytes are ameliorated by increasing hexokinase 1 expression

Bell

Wareing

Hamshaw

et al. 2023

Preprint

Self Cite

View full text Add to dashboard Cite

show abstract

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Oxidative switch drives mitophagy defects in dopaminergicparkinmutant patient neurons

Cited by 1 publication

References 44 publications

Deficits in mitochondrial function and glucose metabolism seen in sporadic and familial Alzheimer’s disease derived Astrocytes are ameliorated by increasing hexokinase 1 expression

Deficits in mitochondrial function and glucose metabolism seen in sporadic and familial Alzheimer’s disease derived Astrocytes are ameliorated by increasing hexokinase 1 expression

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