Myogenesis defects in a patient-derived iPSC model of hereditary GNE myopathy

Hereditary muscle diseases are disabling disorders lacking effective treatments. UDP-N-acetylglucosamine-2-epimerase/N-acetylmannosamine kinase (GNE) myopathy (GNEM) is an autosomal recessive distal myopathy with rimmed vacuoles typically manifesting in late adolescence/early adulthood. GNE encodes...

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Published innpj Regenerative medicine Vol. 7; no. 1; p. 48
Main Authors Schmitt, Rebecca E., Smith, Douglas Y., Cho, Dong Seong, Kirkeby, Lindsey A., Resch, Zachary T., Liewluck, Teerin, Niu, Zhiyv, Milone, Margherita, Doles, Jason D.
Format Journal Article
LanguageEnglish
Published London Nature Publishing Group UK 09.09.2022
Nature Publishing Group
Nature Portfolio
Subjects
631/80/304
692/699/317
Acids
Autophagy
Biomaterials
Biomedical and Life Sciences
Biomedicine
Biopsy
Biosynthesis
Cell Biology
Disease
Electromyography
Genotype & phenotype
Immunology
Kinases
Medical research
Musculoskeletal system
Mutation
Myogenesis
Phosphatase
Proteins
Regenerative medicine
Regenerative Medicine/Tissue Engineering
Stem Cells
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Summary:Hereditary muscle diseases are disabling disorders lacking effective treatments. UDP-N-acetylglucosamine-2-epimerase/N-acetylmannosamine kinase (GNE) myopathy (GNEM) is an autosomal recessive distal myopathy with rimmed vacuoles typically manifesting in late adolescence/early adulthood. GNE encodes the rate-limiting enzyme in sialic acid biosynthesis, which is necessary for the proper function of numerous biological processes. Outside of the causative gene, very little is known about the mechanisms contributing to the development of GNE myopathy. In the present study, we aimed to address this knowledge gap by querying the underlying mechanisms of GNE myopathy using a patient-derived induced pluripotent stem-cell (iPSC) model. Control and patient-specific iPSCs were differentiated down a skeletal muscle lineage, whereby patient-derived GNEM iPSC clones were able to recapitulate key characteristics of the human pathology and further demonstrated defects in myogenic progression. Single-cell RNA sequencing time course studies revealed clear differences between control and GNEM iPSC-derived muscle precursor cells (iMPCs), while pathway studies implicated altered stress and autophagy signaling in GNEM iMPCs. Treatment of GNEM patient-derived iMPCs with an autophagy activator improved myogenic differentiation. In summary, we report an in vitro, iPSC-based model of GNE myopathy and implicate defective myogenesis as a contributing mechanism to the etiology of GNE myopathy.
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ISSN:2057-3995
2057-3995
DOI:10.1038/s41536-022-00238-3