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ApoE4-dependent lysosomal cholesterol accumulation impairs mitochondrial homeostasis and oxidative phosphorylation in human astrocytes

Title
ApoE4-dependent lysosomal cholesterol accumulation impairs mitochondrial homeostasis and oxidative phosphorylation in human astrocytes
Author(s)
Lee, HyeinCho, SukheeKim, Mi-JinPark, Yeo JinCho, EunjiJo, Yeon SukKim, Yong-SeokLee, Jung YiThoudam, ThemisWoo, Seung-HwaLee, Se-InJeon, JuyeongLee, Young-SamSuh, Byung-ChangYoon, Jong HyukGo, YounghoonLee, In-KyuSeo, Jinsoo
Issued Date
2023-10
Citation
Cell Reports, v.42, no.10
Type
Article
Author Keywords
ApoE4CP: Cell biologyCP: Metabolismglucose metabolismhuman astrocyteslysosomal cholesterol accumulationmitophagy
Keywords
BRAIN AEROBIC GLYCOLYSISMETHYL-BETA-CYCLODEXTRINALZHEIMERS-DISEASEPATTERNSAPOE
ISSN
2211-1247
Abstract
Recent developments in genome sequencing have expanded the knowledge of genetic factors associated with late-onset Alzheimer's disease (AD). Among them, genetic variant ε4 of the APOE gene (APOE4) confers the greatest disease risk. Dysregulated glucose metabolism is an early pathological feature of AD. Using isogenic ApoE3 and ApoE4 astrocytes derived from human induced pluripotent stem cells, we find that ApoE4 increases glycolytic activity but impairs mitochondrial respiration in astrocytes. Ultrastructural and autophagy flux analyses show that ApoE4-induced cholesterol accumulation impairs lysosome-dependent removal of damaged mitochondria. Acute treatment with cholesterol-depleting agents restores autophagic activity, mitochondrial dynamics, and associated proteomes, and extended treatment rescues mitochondrial respiration in ApoE4 astrocytes. Taken together, our study provides a direct link between ApoE4-induced lysosomal cholesterol accumulation and abnormal oxidative phosphorylation. © 2023 The Author(s)
URI
http://hdl.handle.net/20.500.11750/46661
DOI
10.1016/j.celrep.2023.113183
Publisher
Cell Press
Related Researcher
  • 이영삼 Lee, Young-Sam
  • Research Interests DNA replication and repair; Restoration of cellular senescence; Structural and functional relationship of proteins
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Appears in Collections:
Department of New Biology Senescence-Associated Mechanism Lab 1. Journal Articles
Department of Brain Sciences Laboratory of Aging Brain 1. Journal Articles
Department of Brain Sciences Laboratory of Brain Signal and Synapse Research 1. Journal Articles

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