Hallmark Molecular and Pathological Features of POLG Disease are Recapitulated in Cerebral Organoids

Anbin Chen; Tsering Yangzom; Yu Hong; Bjørn Christian Lundberg; Gareth John Sullivan; Charalampos Tzoulis; Laurence A. Bindoff; Kristina Xiao Liang

doi:10.1002/advs.202307136

Advanced Science (May 2024)

Hallmark Molecular and Pathological Features of POLG Disease are Recapitulated in Cerebral Organoids

Anbin Chen,
Tsering Yangzom,
Yu Hong,
Bjørn Christian Lundberg,
Gareth John Sullivan,
Charalampos Tzoulis,
Laurence A. Bindoff,
Kristina Xiao Liang

Affiliations

Anbin Chen: Department of Clinical Medicine (K1) University of Bergen Bergen 5021 Norway
Tsering Yangzom: Department of Clinical Medicine (K1) University of Bergen Bergen 5021 Norway
Yu Hong: Department of Clinical Medicine (K1) University of Bergen Bergen 5021 Norway
Bjørn Christian Lundberg: Department of Clinical Medicine (K1) University of Bergen Bergen 5021 Norway
Gareth John Sullivan: Department of Pediatric Research Oslo University Hospital Oslo 0424 Norway
Charalampos Tzoulis: Department of Clinical Medicine (K1) University of Bergen Bergen 5021 Norway
Laurence A. Bindoff: Department of Clinical Medicine (K1) University of Bergen Bergen 5021 Norway
Kristina Xiao Liang: Department of Clinical Medicine (K1) University of Bergen Bergen 5021 Norway

DOI: https://doi.org/10.1002/advs.202307136
Journal volume & issue: Vol. 11, no. 18
pp. n/a – n/a

Abstract

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Abstract In this research, a 3D brain organoid model is developed to study POLG‐related encephalopathy, a mitochondrial disease stemming from POLG mutations. Induced pluripotent stem cells (iPSCs) derived from patients with these mutations is utilized to generate cortical organoids, which exhibited typical features of the diseases with POLG mutations, such as altered morphology, neuronal loss, and mitochondiral DNA (mtDNA) depletion. Significant dysregulation is also identified in pathways crucial for neuronal development and function, alongside upregulated NOTCH and JAK‐STAT signaling pathways. Metformin treatment ameliorated many of these abnormalities, except for the persistent affliction of inhibitory dopamine‐glutamate (DA GLU) neurons. This novel model effectively mirrors both the molecular and pathological attributes of diseases with POLG mutations, providing a valuable tool for mechanistic understanding and therapeutic screening for POLG‐related disorders and other conditions characterized by compromised neuronal mtDNA maintenance and complex I deficiency.

Published in Advanced Science

ISSN: 2198-3844 (Online)
Publisher: Wiley
Country of publisher: Germany
LCC subjects: Science
Website: https://onlinelibrary.wiley.com/journal/21983844

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