Gene expression profiling of skeletal myogenesis in human embryonic stem cells reveals a potential cascade of transcription factors regulating stages of myogenesis, including quiescent/activated satellite cell-like gene expression

Human embryonic stem cell (hESC)-derived skeletal muscle progenitors (SMP)—defined as PAX7-expressing cells with myogenic potential—can provide an abundant source of donor material for muscle stem cell therapy. As in vitro myogenesis is decoupled from in vivo timing and 3D-embryo structure, it is im...

Descripción completa

Detalles Bibliográficos
Autores principales: Shelton, Michael, Ritso, Morten, Liu, Jun, O’Neil, Daniel, Kocharyan, Avetik, Rudnicki, Michael A., Stanford, William L., Skerjanc, Ilona S., Blais, Alexandre
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2019
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6764674/
https://www.ncbi.nlm.nih.gov/pubmed/31560727
http://dx.doi.org/10.1371/journal.pone.0222946
_version_ 1783454424959549440
author Shelton, Michael
Ritso, Morten
Liu, Jun
O’Neil, Daniel
Kocharyan, Avetik
Rudnicki, Michael A.
Stanford, William L.
Skerjanc, Ilona S.
Blais, Alexandre
author_facet Shelton, Michael
Ritso, Morten
Liu, Jun
O’Neil, Daniel
Kocharyan, Avetik
Rudnicki, Michael A.
Stanford, William L.
Skerjanc, Ilona S.
Blais, Alexandre
author_sort Shelton, Michael
collection PubMed
description Human embryonic stem cell (hESC)-derived skeletal muscle progenitors (SMP)—defined as PAX7-expressing cells with myogenic potential—can provide an abundant source of donor material for muscle stem cell therapy. As in vitro myogenesis is decoupled from in vivo timing and 3D-embryo structure, it is important to characterize what stage or type of muscle is modeled in culture. Here, gene expression profiling is analyzed in hESCs over a 50 day skeletal myogenesis protocol and compared to datasets of other hESC-derived skeletal muscle and adult murine satellite cells. Furthermore, day 2 cultures differentiated with high or lower concentrations of CHIR99021, a GSK3A/GSK3B inhibitor, were contrasted. Expression profiling of the 50 day time course identified successively expressed gene subsets involved in mesoderm/paraxial mesoderm induction, somitogenesis, and skeletal muscle commitment/formation which could be regulated by a putative cascade of transcription factors. Initiating differentiation with higher CHIR99021 concentrations significantly increased expression of MSGN1 and TGFB-superfamily genes, notably NODAL, resulting in enhanced paraxial mesoderm and reduced ectoderm/neuronal gene expression. Comparison to adult satellite cells revealed that genes expressed in 50-day cultures correlated better with those expressed by quiescent or early activated satellite cells, which have the greatest therapeutic potential. Day 50 cultures were similar to other hESC-derived skeletal muscle and both expressed known and novel SMP surface proteins. Overall, a putative cascade of transcription factors has been identified which regulates four stages of myogenesis. Subsets of these factors were upregulated by high CHIR99021 or their binding sites were significantly over-represented during SMP activation, ranging from quiescent to late-activated stages. This analysis serves as a resource to further study the progression of in vitro skeletal myogenesis and could be mined to identify novel markers of pluripotent-derived SMPs or regulatory transcription/growth factors. Finally, 50-day hESC-derived SMPs appear similar to quiescent/early activated satellite cells, suggesting they possess therapeutic potential.
format Online
Article
Text
id pubmed-6764674
institution National Center for Biotechnology Information
language English
publishDate 2019
publisher Public Library of Science
record_format MEDLINE/PubMed
spelling pubmed-67646742019-10-12 Gene expression profiling of skeletal myogenesis in human embryonic stem cells reveals a potential cascade of transcription factors regulating stages of myogenesis, including quiescent/activated satellite cell-like gene expression Shelton, Michael Ritso, Morten Liu, Jun O’Neil, Daniel Kocharyan, Avetik Rudnicki, Michael A. Stanford, William L. Skerjanc, Ilona S. Blais, Alexandre PLoS One Research Article Human embryonic stem cell (hESC)-derived skeletal muscle progenitors (SMP)—defined as PAX7-expressing cells with myogenic potential—can provide an abundant source of donor material for muscle stem cell therapy. As in vitro myogenesis is decoupled from in vivo timing and 3D-embryo structure, it is important to characterize what stage or type of muscle is modeled in culture. Here, gene expression profiling is analyzed in hESCs over a 50 day skeletal myogenesis protocol and compared to datasets of other hESC-derived skeletal muscle and adult murine satellite cells. Furthermore, day 2 cultures differentiated with high or lower concentrations of CHIR99021, a GSK3A/GSK3B inhibitor, were contrasted. Expression profiling of the 50 day time course identified successively expressed gene subsets involved in mesoderm/paraxial mesoderm induction, somitogenesis, and skeletal muscle commitment/formation which could be regulated by a putative cascade of transcription factors. Initiating differentiation with higher CHIR99021 concentrations significantly increased expression of MSGN1 and TGFB-superfamily genes, notably NODAL, resulting in enhanced paraxial mesoderm and reduced ectoderm/neuronal gene expression. Comparison to adult satellite cells revealed that genes expressed in 50-day cultures correlated better with those expressed by quiescent or early activated satellite cells, which have the greatest therapeutic potential. Day 50 cultures were similar to other hESC-derived skeletal muscle and both expressed known and novel SMP surface proteins. Overall, a putative cascade of transcription factors has been identified which regulates four stages of myogenesis. Subsets of these factors were upregulated by high CHIR99021 or their binding sites were significantly over-represented during SMP activation, ranging from quiescent to late-activated stages. This analysis serves as a resource to further study the progression of in vitro skeletal myogenesis and could be mined to identify novel markers of pluripotent-derived SMPs or regulatory transcription/growth factors. Finally, 50-day hESC-derived SMPs appear similar to quiescent/early activated satellite cells, suggesting they possess therapeutic potential. Public Library of Science 2019-09-27 /pmc/articles/PMC6764674/ /pubmed/31560727 http://dx.doi.org/10.1371/journal.pone.0222946 Text en © 2019 Shelton et al http://creativecommons.org/licenses/by/4.0/ This is an open access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Article
Shelton, Michael
Ritso, Morten
Liu, Jun
O’Neil, Daniel
Kocharyan, Avetik
Rudnicki, Michael A.
Stanford, William L.
Skerjanc, Ilona S.
Blais, Alexandre
Gene expression profiling of skeletal myogenesis in human embryonic stem cells reveals a potential cascade of transcription factors regulating stages of myogenesis, including quiescent/activated satellite cell-like gene expression
title Gene expression profiling of skeletal myogenesis in human embryonic stem cells reveals a potential cascade of transcription factors regulating stages of myogenesis, including quiescent/activated satellite cell-like gene expression
title_full Gene expression profiling of skeletal myogenesis in human embryonic stem cells reveals a potential cascade of transcription factors regulating stages of myogenesis, including quiescent/activated satellite cell-like gene expression
title_fullStr Gene expression profiling of skeletal myogenesis in human embryonic stem cells reveals a potential cascade of transcription factors regulating stages of myogenesis, including quiescent/activated satellite cell-like gene expression
title_full_unstemmed Gene expression profiling of skeletal myogenesis in human embryonic stem cells reveals a potential cascade of transcription factors regulating stages of myogenesis, including quiescent/activated satellite cell-like gene expression
title_short Gene expression profiling of skeletal myogenesis in human embryonic stem cells reveals a potential cascade of transcription factors regulating stages of myogenesis, including quiescent/activated satellite cell-like gene expression
title_sort gene expression profiling of skeletal myogenesis in human embryonic stem cells reveals a potential cascade of transcription factors regulating stages of myogenesis, including quiescent/activated satellite cell-like gene expression
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6764674/
https://www.ncbi.nlm.nih.gov/pubmed/31560727
http://dx.doi.org/10.1371/journal.pone.0222946
work_keys_str_mv AT sheltonmichael geneexpressionprofilingofskeletalmyogenesisinhumanembryonicstemcellsrevealsapotentialcascadeoftranscriptionfactorsregulatingstagesofmyogenesisincludingquiescentactivatedsatellitecelllikegeneexpression
AT ritsomorten geneexpressionprofilingofskeletalmyogenesisinhumanembryonicstemcellsrevealsapotentialcascadeoftranscriptionfactorsregulatingstagesofmyogenesisincludingquiescentactivatedsatellitecelllikegeneexpression
AT liujun geneexpressionprofilingofskeletalmyogenesisinhumanembryonicstemcellsrevealsapotentialcascadeoftranscriptionfactorsregulatingstagesofmyogenesisincludingquiescentactivatedsatellitecelllikegeneexpression
AT oneildaniel geneexpressionprofilingofskeletalmyogenesisinhumanembryonicstemcellsrevealsapotentialcascadeoftranscriptionfactorsregulatingstagesofmyogenesisincludingquiescentactivatedsatellitecelllikegeneexpression
AT kocharyanavetik geneexpressionprofilingofskeletalmyogenesisinhumanembryonicstemcellsrevealsapotentialcascadeoftranscriptionfactorsregulatingstagesofmyogenesisincludingquiescentactivatedsatellitecelllikegeneexpression
AT rudnickimichaela geneexpressionprofilingofskeletalmyogenesisinhumanembryonicstemcellsrevealsapotentialcascadeoftranscriptionfactorsregulatingstagesofmyogenesisincludingquiescentactivatedsatellitecelllikegeneexpression
AT stanfordwilliaml geneexpressionprofilingofskeletalmyogenesisinhumanembryonicstemcellsrevealsapotentialcascadeoftranscriptionfactorsregulatingstagesofmyogenesisincludingquiescentactivatedsatellitecelllikegeneexpression
AT skerjancilonas geneexpressionprofilingofskeletalmyogenesisinhumanembryonicstemcellsrevealsapotentialcascadeoftranscriptionfactorsregulatingstagesofmyogenesisincludingquiescentactivatedsatellitecelllikegeneexpression
AT blaisalexandre geneexpressionprofilingofskeletalmyogenesisinhumanembryonicstemcellsrevealsapotentialcascadeoftranscriptionfactorsregulatingstagesofmyogenesisincludingquiescentactivatedsatellitecelllikegeneexpression

Ejemplares similares