Disease‐specific phenotypes in
            <scp>iPSC</scp>
            ‐derived neural stem cells with
            <i>
              <scp>POLG</scp>
            </i>
            mutations

Liang, Kristina Xiao; Kristiansen, Cecilie Katrin; Mostafavi, Sepideh; Vatne, Guro Helén; Zantingh, Gina Alien; Kianian, Atefeh; Tzoulis, Charalampos; Høyland, Lena Elise; Ziegler, Mathias; Pérez, Ricardo; Furriol, Jessica; Zhang, Zhuoyuan; Balafkan, Novin; Hong, Yu; Siller, Richard; Sullivan, Gareth J.; Bindoff, Laurence A.

doi:10.15252/emmm.202012146

Cited by 41 publications

(74 citation statements)

References 75 publications

(113 reference statements)

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“…In micro-dissected post-mortem neurons, we showed previously that respiratory chain complex I was lost in POLG affected frontal and cerebellar neurons [2] and we subsequently confirmed this in iPSCderived neural stem cells (NSCs) and iPSC-derived dopaminergic (DA) neurons [19]. We, therefore, investigated the levels of each respiratory chain complex in our astrocytes using flow cytometry, immunohistochemistry, and western blotting.…”

Section: Polg-astrocytes Display a Loss Of Complex I And Ivmentioning

confidence: 60%

“…4h & i), although WS5A astrocytes did not reach significance. These data indicate that the respiratory chain defect in astrocytes carrying POLG mutations appears more extensive than that seen in post-mortem neurons [23] and neuronal stem cells derived from the same iPSCs [19], where only loss of complex I was identified. A decreased expression of voltagedependent anion channels (VDAC), located in the mitochondrial outer membrane, was also identified in WS5A and CP2A astrocytes compared to controls, although it failed to reach significance ( Fig.…”

Section: Polg-astrocytes Display a Loss Of Complex I And Ivmentioning

confidence: 79%

“…We generated patient iPSCs (Table S1) as previously described [19] using fibroblasts of two patients, one homozygous for c.2243G>C; p.W748S (WS5A) and one compound heterozygous c.1399G>A/c.2243G>C; p.A467T/W748S (CP2A). Control iPSCs were generated from two normal human fibroblast lines, Detroit 551 and AG05836B.…”

Section: Resultsmentioning

confidence: 99%

“…To generate patient and control astrocytes ( Fig. 1a), we first generated neural stem cells (NSCs) using a previously published protocol [19]. Within 5 days of induction, iPSC cells (Fig.…”

Section: Resultsmentioning

confidence: 99%

“…Previous studies, including our own in post-mortem tissue [2] and NSCs [19], have focused on the neuronal consequences of POLG mutations. Here, we show, for the first time, that mitochondrial defects including decreased membrane potential, respiratory chain complex loss, lowered ATP levels and mtDNA depletion also occur in iPSC-derived astrocytes.…”

Section: Insert the Red Ones From Version In Nature Neuronsciencementioning

confidence: 99%

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Stem cell derived astrocytes withPOLGmutations and mitochondrial dysfunction including abnormal NAD+ metabolism is toxic for neurons

Liang

Kianian

Chen

et al. 2020

Preprint

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The inability to reliably replicate mitochondrial DNA (mtDNA) by mitochondrial DNA polymerase gamma (POLG) leads to a subset of common mitochondrial diseases associated with neuronal death and depletion of neuronal mtDNA. Defining disease mechanisms remains difficult due to the limited access to human tissue. Astrocytes are highly abundant in the brain, playing a crucial role in the support and modulation of neuronal function. Astrocytes also respond to insults affecting the brain. Following damage to the center neural system, which can be hypoxia, inflammation or neurodegeneration, astrocytes become activated, lose their supportive role and gain toxic functions that induce rapid death of neurons and oligodendrocytes. The role of astrocyte reactivation and the consequences this has for neuronal homeostasis in mitochondrial diseases has not been explored. Here, using patient cells carrying POLG mutations, we generated iPSCs and then differentiated into astrocytes. We demonstrated that POLG-astrocytes exhibited both mitochondrial dysfunctions, including loss of mitochondrial membrane potential, energy failure, complex I and IV defects, disturbed NAD+/NADH metabolism, and mtDNA depletion. Further, POLG derived astrocytes presented an A1-like reactive phenotype with increased proliferation, invasion, upregulation of pathways involved in response to stimulus, immune system process, cell proliferation and cell killing. Under direct and indirect co-culture with neurons, POLG-astrocytes exhibited a toxic effect leading to the death of neurons. Our findings demonstrate that mitochondrial dysfunction caused by POLG mutations leads not only to intrinsic defects in energy metabolism affecting both neurons and astrocytes, but also to neurotoxic damage driven by astrocytes. Our studies provide a robust astroglia-neuron interaction model for future investigation of mitochondrial involvement in neurogenesis and neurodegenerative diseases.

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Section: Polg-astrocytes Display a Loss Of Complex I And Ivmentioning

confidence: 60%

Section: Polg-astrocytes Display a Loss Of Complex I And Ivmentioning

confidence: 79%

Section: Resultsmentioning

confidence: 99%

“…To generate patient and control astrocytes ( Fig. 1a), we first generated neural stem cells (NSCs) using a previously published protocol [19]. Within 5 days of induction, iPSC cells (Fig.…”

Section: Resultsmentioning

confidence: 99%

Section: Insert the Red Ones From Version In Nature Neuronsciencementioning

confidence: 99%

See 3 more Smart Citations

Stem cell derived astrocytes withPOLGmutations and mitochondrial dysfunction including abnormal NAD+ metabolism is toxic for neurons

Liang

Kianian

Chen

et al. 2020

Preprint

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Human induced pluripotent stem cells for studying mitochondrial diseases in the heart

Caudal

Ren

et al. 2022

FEBS Letters

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Mitochondrial dysfunction is known to contribute to a range of diseases, and primary mitochondrial defects strongly impact high‐energy organs such as the heart. Platforms for high‐throughput and human‐relevant assessment of mitochondrial diseases are currently lacking, hindering the development of targeted therapies. In the past decade, human‐induced pluripotent stem cells (iPSCs) have become a promising technology for drug discovery in basic and clinical research. In particular, human iPSC‐derived cardiomyocytes (iPSC‐CMs) offer a unique tool to study a wide range of mitochondrial functions and possess the potential to become a key translational asset for mitochondrial drug development. This review summarizes mitochondrial functions and recent therapeutic discoveries, advancements and limitations of using iPSC‐CMs to study mitochondrial diseases of the heart with an emphasis on cardiac applications.

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

Chen,

Yangzom,

Hong

et al. 2024

Advanced Science

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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.

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Disease‐specific phenotypes in iPSC ‐derived neural stem cells with POLG mutations

Cited by 41 publications

References 75 publications

Stem cell derived astrocytes withPOLGmutations and mitochondrial dysfunction including abnormal NAD+ metabolism is toxic for neurons

Stem cell derived astrocytes withPOLGmutations and mitochondrial dysfunction including abnormal NAD+ metabolism is toxic for neurons

Human induced pluripotent stem cells for studying mitochondrial diseases in the heart

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

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