ERBB3 and NGFR mark a distinct skeletal muscle progenitor cell in human development and hPSCs.
Michael R HicksJulia HiserodtKatrina ParasWakana FujiwaraAscia EskinMajib JanHaibin XiCourtney S YoungDenis EvseenkoStanley F NelsonMelissa J SpencerBen Van HandelApril D PylePublished in: Nature cell biology (2017)
Human pluripotent stem cells (hPSCs) can be directed to differentiate into skeletal muscle progenitor cells (SMPCs). However, the myogenicity of hPSC-SMPCs relative to human fetal or adult satellite cells remains unclear. We observed that hPSC-SMPCs derived by directed differentiation are less functional in vitro and in vivo compared to human satellite cells. Using RNA sequencing, we found that the cell surface receptors ERBB3 and NGFR demarcate myogenic populations, including PAX7 progenitors in human fetal development and hPSC-SMPCs. We demonstrated that hPSC skeletal muscle is immature, but inhibition of transforming growth factor-β signalling during differentiation improved fusion efficiency, ultrastructural organization and the expression of adult myosins. This enrichment and maturation strategy restored dystrophin in hundreds of dystrophin-deficient myofibres after engraftment of CRISPR-Cas9-corrected Duchenne muscular dystrophy human induced pluripotent stem cell-SMPCs. The work provides an in-depth characterization of human myogenesis, and identifies candidates that improve the in vivo myogenic potential of hPSC-SMPCs to levels that are equal to directly isolated human fetal muscle cells.
Keyphrases
- pluripotent stem cells
- endothelial cells
- skeletal muscle
- duchenne muscular dystrophy
- induced pluripotent stem cells
- crispr cas
- stem cells
- induced apoptosis
- transforming growth factor
- insulin resistance
- metabolic syndrome
- poor prognosis
- gene expression
- epithelial mesenchymal transition
- long non coding rna
- cell cycle arrest
- young adults
- risk assessment
- genome wide
- cell proliferation
- binding protein
- cord blood