Amyloid-β Oligomers-induced Mitochondrial DNA Repair Impairment Contributes to Altered Human Neural Stem Cell Differentiation

Jing Lu; Yi Li; Cristiana Mollinari; Enrico Garaci; Daniela Merlo; Gang Pei

doi:10.2174/1567205016666191023104036

Amyloid-β Oligomers-induced Mitochondrial DNA Repair Impairment Contributes to Altered Human Neural Stem Cell Differentiation

Curr Alzheimer Res. 2019;16(10):934-949. doi: 10.2174/1567205016666191023104036.

Authors

Jing Lu¹, Yi Li^{1

2}, Cristiana Mollinari^{3

4}, Enrico Garaci^{5

6}, Daniela Merlo³, Gang Pei^{1

7

8}

Affiliations

¹ State Key Laboratory of Cell Biology, CAS Center for Excellence in Molecular Cell Science, Shanghai Institute of Biochemistry and Cell Biology, Chinese Academy of Sciences, University of Chinese Academy of Sciences, 320 Yueyang Road, Shanghai 200031, China.
² School of Life Science and Technology, ShanghaiTech University, 100 Haike Road, Shanghai 201210, China.
³ Department of Neuroscience, Istituto Superiore di Sanita, Rome, Italy.
⁴ Institute of Translational Pharmacology, National Research Council, Rome, Italy.
⁵ IRCCS San Raffaele Pisana, Via di Val Cannuta 247, 00166 Rome, Italy.
⁶ Telematic University San Raffaele, Via di Val Cannuta 247, 00166 Rome, Italy.
⁷ Shanghai Key Laboratory of Signaling and Disease Research, Collaborative Innovation Center for Brain Science, School of Life Sciences and Technology, Tongji University, Shanghai, China.
⁸ Institute for Stem Cell and Regeneration, Chinese Academy of Sciences, Beijing, China.

PMID: 31642778
DOI: 10.2174/1567205016666191023104036

Abstract

Background: Amyloid-β42 oligomers (Aβ42O), the proximate effectors of neurotoxicity observed in Alzheimer's disease (AD), can induce mitochondrial oxidative stress and impair mitochondrial function besides causing mitochondrial DNA (mtDNA) damage. Aβ42O also regulate the proliferative and differentiative properties of stem cells.

Objective: We aimed to study whether Aβ42O-induced mtDNA damage is involved in the regulation of stem cell differentiation.

Method: Human iPSCs-derived neural stem cell (NSC) was applied to investigate the effect of Aβ42O on reactive oxygen species (ROS) production and DNA damage using mitoSOX staining and long-range PCR lesion assay, respectively. mtDNA repair activity was measured by non-homologous end joining (NHEJ) in vitro assay using mitochondria isolates and the expression and localization of NHEJ components were determined by Western blot and immunofluorescence assay. The expressions of Tuj-1 and GFAP, detected by immunofluorescence and qPCR, respectively, were examined as an index of neurons and astrocytes production.

Results: We show that in NSC Aβ42O treatment induces ROS production and mtDNA damage and impairs DNA end joining activity. NHEJ components, such as Ku70/80, DNA-PKcs, and XRCC4, are localized in mitochondria and silencing of XRCC4 significantly exacerbates the effect of Aβ42O on mtDNA integrity. On the contrary, pre-treatment with Phytic Acid (IP6), which specifically stimulates DNA-PK-dependent end-joining, inhibits Aβ42O-induced mtDNA damage and neuronal differentiation alteration.

Conclusion: Aβ42O-induced mtDNA repair impairment may change cell fate thus shifting human NSC differentiation toward an astrocytic lineage. Repair stimulation counteracts Aβ42O neurotoxicity, suggesting mtDNA repair pathway as a potential target for the treatment of neurodegenerative disorders like AD.

Keywords: Amyloid-β; DNA damage; DNA repair; differentiation; human neural stem cell; mitochondria..

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Amyloid beta-Peptides / toxicity*
Cell Differentiation / drug effects
Cell Differentiation / physiology*
DNA Repair / drug effects
DNA Repair / physiology*
DNA, Mitochondrial / metabolism*
Humans
Induced Pluripotent Stem Cells / drug effects
Induced Pluripotent Stem Cells / metabolism*
Neural Stem Cells / drug effects
Neural Stem Cells / metabolism*
Peptide Fragments / toxicity*

Substances

Amyloid beta-Peptides
DNA, Mitochondrial
Peptide Fragments
amyloid beta-protein (1-42)