Direct genesis of functional rodent and human schwann cells from skin mesenchymal precursors

Matthew P. Krause; Shaalee Dworski; Konstantin Feinberg; Karen Jones; Adam P.W. Johnston; Smitha Paul; Maryline Paris; Elior Peles; Darius Bagli; Christopher R. Forrest; David R. Kaplan; Freda D. Miller

doi:10.1016/j.stemcr.2014.05.011

Direct genesis of functional rodent and human schwann cells from skin mesenchymal precursors

Matthew P. Krause, Shaalee Dworski, Konstantin Feinberg, Karen Jones, Adam P.W. Johnston, Smitha Paul, Maryline Paris, Elior Peles, Darius Bagli, Christopher R. Forrest, David R. Kaplan, Freda D. Miller

Department of Molecular Cell Biology

Weizmann Institute of Science

Research output: Contribution to journal › Article › peer-review

Abstract

Recent reports of directed reprogramming have raised questions about the stability of cell lineages. Here, we have addressed this issue, focusing upon skin-derived precursors (SKPs), a dermally derived precursor cell. We show by lineage tracing that murine SKPs from dorsal skin originate from mesenchymal and not neural crest-derived cells. These mesenchymally derived SKPs can, without genetic manipulation, generate functional Schwann cells, a neural crest cell type, and are highly similar at the transcriptional level to Schwann cells isolated from the peripheral nerve. This is not a mouse-specific phenomenon, since human SKPs that are highly similar at the transcriptome level can be made from neural crest-derived facial and mesodermally derived foreskin dermis and the foreskin SKPs can make myelinating Schwann cells. Thus, nonneural crest-derived mesenchymal precursors can differentiate into bona fide peripheral glia in the absence of genetic manipulation, suggesting that developmentally defined lineage boundaries are more flexible than widely thought.

Original language	English
Pages (from-to)	85-100
Number of pages	16
Journal	Stem Cell Reports
Volume	3
Issue number	1
DOIs	https://doi.org/10.1016/j.stemcr.2014.05.011
State	Published - 8 Jul 2014

All Science Journal Classification (ASJC) codes

Biochemistry
Genetics
Developmental Biology
Cell Biology

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10.1016/j.stemcr.2014.05.011

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title = "Direct genesis of functional rodent and human schwann cells from skin mesenchymal precursors",

abstract = "Recent reports of directed reprogramming have raised questions about the stability of cell lineages. Here, we have addressed this issue, focusing upon skin-derived precursors (SKPs), a dermally derived precursor cell. We show by lineage tracing that murine SKPs from dorsal skin originate from mesenchymal and not neural crest-derived cells. These mesenchymally derived SKPs can, without genetic manipulation, generate functional Schwann cells, a neural crest cell type, and are highly similar at the transcriptional level to Schwann cells isolated from the peripheral nerve. This is not a mouse-specific phenomenon, since human SKPs that are highly similar at the transcriptome level can be made from neural crest-derived facial and mesodermally derived foreskin dermis and the foreskin SKPs can make myelinating Schwann cells. Thus, nonneural crest-derived mesenchymal precursors can differentiate into bona fide peripheral glia in the absence of genetic manipulation, suggesting that developmentally defined lineage boundaries are more flexible than widely thought.",

author = "Krause, \{Matthew P.\} and Shaalee Dworski and Konstantin Feinberg and Karen Jones and Johnston, \{Adam P.W.\} and Smitha Paul and Maryline Paris and Elior Peles and Darius Bagli and Forrest, \{Christopher R.\} and Kaplan, \{David R.\} and Miller, \{Freda D.\}",

note = "CIHR [MOP-64211]; Canadian SCN Global Research; Jacobs Ladder Foundation; CIHR; Ontario Stem Cell Initiative; CIHR Training Program in Regenerative MedicineThis work was funded by CIHR grant MOP-64211 and a Canadian SCN Global Research grant to F. D. M. K. F., M. P. K., A.P.W.J., and S. D. are funded by scholarships from the Jacobs Ladder Foundation, CIHR, the Ontario Stem Cell Initiative, and the CIHR Training Program in Regenerative Medicine, respectively. F. D. M. and D. R. K. hold Canada Research Chairs, and F. D. M. is an HHMI Senior International Research Scholar. We thank Benigno Aquino and Vania Ariosa for technical advice and assistance.",

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doi = "10.1016/j.stemcr.2014.05.011",

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T1 - Direct genesis of functional rodent and human schwann cells from skin mesenchymal precursors

AU - Krause, Matthew P.

AU - Dworski, Shaalee

AU - Feinberg, Konstantin

AU - Jones, Karen

AU - Johnston, Adam P.W.

AU - Paul, Smitha

AU - Paris, Maryline

AU - Peles, Elior

AU - Bagli, Darius

AU - Forrest, Christopher R.

AU - Kaplan, David R.

AU - Miller, Freda D.

N1 - CIHR [MOP-64211]; Canadian SCN Global Research; Jacobs Ladder Foundation; CIHR; Ontario Stem Cell Initiative; CIHR Training Program in Regenerative MedicineThis work was funded by CIHR grant MOP-64211 and a Canadian SCN Global Research grant to F. D. M. K. F., M. P. K., A.P.W.J., and S. D. are funded by scholarships from the Jacobs Ladder Foundation, CIHR, the Ontario Stem Cell Initiative, and the CIHR Training Program in Regenerative Medicine, respectively. F. D. M. and D. R. K. hold Canada Research Chairs, and F. D. M. is an HHMI Senior International Research Scholar. We thank Benigno Aquino and Vania Ariosa for technical advice and assistance.

PY - 2014/7/8

Y1 - 2014/7/8

N2 - Recent reports of directed reprogramming have raised questions about the stability of cell lineages. Here, we have addressed this issue, focusing upon skin-derived precursors (SKPs), a dermally derived precursor cell. We show by lineage tracing that murine SKPs from dorsal skin originate from mesenchymal and not neural crest-derived cells. These mesenchymally derived SKPs can, without genetic manipulation, generate functional Schwann cells, a neural crest cell type, and are highly similar at the transcriptional level to Schwann cells isolated from the peripheral nerve. This is not a mouse-specific phenomenon, since human SKPs that are highly similar at the transcriptome level can be made from neural crest-derived facial and mesodermally derived foreskin dermis and the foreskin SKPs can make myelinating Schwann cells. Thus, nonneural crest-derived mesenchymal precursors can differentiate into bona fide peripheral glia in the absence of genetic manipulation, suggesting that developmentally defined lineage boundaries are more flexible than widely thought.

AB - Recent reports of directed reprogramming have raised questions about the stability of cell lineages. Here, we have addressed this issue, focusing upon skin-derived precursors (SKPs), a dermally derived precursor cell. We show by lineage tracing that murine SKPs from dorsal skin originate from mesenchymal and not neural crest-derived cells. These mesenchymally derived SKPs can, without genetic manipulation, generate functional Schwann cells, a neural crest cell type, and are highly similar at the transcriptional level to Schwann cells isolated from the peripheral nerve. This is not a mouse-specific phenomenon, since human SKPs that are highly similar at the transcriptome level can be made from neural crest-derived facial and mesodermally derived foreskin dermis and the foreskin SKPs can make myelinating Schwann cells. Thus, nonneural crest-derived mesenchymal precursors can differentiate into bona fide peripheral glia in the absence of genetic manipulation, suggesting that developmentally defined lineage boundaries are more flexible than widely thought.

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DO - 10.1016/j.stemcr.2014.05.011

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JO - Stem Cell Reports

JF - Stem Cell Reports

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ER -

Direct genesis of functional rodent and human schwann cells from skin mesenchymal precursors

Abstract

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