4.7 Article

Induced pluripotent stem cell-derived motor neurons of CMT type 2 patients reveal progressive mitochondrial dysfunction

BRAIN (2021)

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Journal

BRAIN
Volume 144, Issue -, Pages 2471-2485

Publisher

OXFORD UNIV PRESS
DOI: 10.1093/brain/awab226

Keywords

Charcot-Marie-Tooth neuropathy; iPSC-derived motor and sensory neurons; phenotyping; mitochondrial dysfunction; dual leucine kinase inhibitor

Categories

Clinical Neurology Neurosciences

Funding

  1. University of Antwerp [38694, 41739, HBC.2016.0534]
  2. Fund for Scientific Research (FWO-Flanders research grant) [G041416N, G017618N]
  3. Fund for Scientific Research (FWO postdoc fellowship)
  4. Association Belge contre les Maladies Neuromusculaires (ABMM grants)
  5. Medical Foundation Queen Elisabeth (GSKE grant)
  6. American Muscular Dystrophy Association (MDA research grant ) [577497]
  7. EU [2012-305121, 779257]
  8. FWO-HERCULES large infrastructure grants [23714, 25340]
  9. University of Antwerp Basic Research Infrastructure grant [41438]

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The study using iPSCs derived from CMT2 patients revealed shared hallmarks of axonal degeneration among different subtypes, suggesting that targeting these common pathomechanisms could lead to the development of a uniform treatment for CMT2.
Axonal Charcot-Marie-Tooth neuropathies (CMT type 2) are caused by inherited mutations in various genes functioning in different pathways. The types of genes and multiplicity of mutations reflect the clinical and genetic heterogeneity in CMT2 disease, which complicates its diagnosis and has inhibited the development of therapies. Here, we used CMT2 patient-derived pluripotent stem cells (iPSCs) to identify common hallmarks of axonal degeneration shared by different CMT2 subtypes. We compared the cellular phenotypes of neurons differentiated from CMT2 patient iPSCs with those from healthy controls and a CRISPR/Cas9-corrected isogenic line. Our results demonstrated neurite network alterations along with extracellular electrophysiological abnormalities in the differentiated motor neurons. Progressive deficits in mitochondrial and lysosomal trafficking, as well as in mitochondrial morphology, were observed in all CMT2 patient lines. Differentiation of the same CMT2 iPSC lines into peripheral sensory neurons only gave rise to cellular phenotypes in subtypes with sensory involvement, supporting the notion that some gene mutations predominantly affect motor neurons. We revealed a common mitochondrial dysfunction in CMT2-derived motor neurons, supported by alterations in the expression pattern and oxidative phosphorylation, which could be recapitulated in the sciatic nerve tissue of a symptomatic mouse model. Inhibition of a dual leucine zipper kinase could partially ameliorate the mitochondrial disease phenotypes in CMT2 subtypes. Altogether, our data reveal shared cellular phenotypes across different CMT2 subtypes and suggests that targeting such common pathomechanisms could allow the development of a uniform treatment for CMT2.

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