Notch controls embryonic Schwann cell differentiation, postnatal myelination and adult plasticity

A Woodhoo; MBD Alonso; A Droggiti; M Turmaine; M D'Antonio; DB Parkinson; DK Wilton; R Al-Shawi; P Simons; J Shen; F Guillemot; F Radtke; Dies Meijer; ML Feltri; L Wrabetz; R Mirsky; KR Jessen

doi:10.1038/nn.2323

Notch controls embryonic Schwann cell differentiation, postnatal myelination and adult plasticity

A Woodhoo, MBD Alonso, A Droggiti, M Turmaine, M D'Antonio, DB Parkinson, DK Wilton, R Al-Shawi, P Simons, J Shen, F Guillemot, F Radtke, Dies Meijer, ML Feltri, L Wrabetz, R Mirsky, KR Jessen

Molecular Genetics

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

244 Citations (Scopus)

Abstract

Notch signaling is central to vertebrate development, and analysis of Notch has provided important insights into pathogenetic mechanisms in the CNS and many other tissues. However, surprisingly little is known about the role of Notch in the development and pathology of Schwann cells and peripheral nerves. Using transgenic mice and cell cultures, we found that Notch has complex and extensive regulatory functions in Schwann cells. Notch promoted the generation of Schwann cells from Schwann cell precursors and regulated the size of the Schwann cell pool by controlling proliferation. Notch inhibited myelination, establishing that myelination is subject to negative transcriptional regulation that opposes forward drives such as Krox20. Notably, in the adult, Notch dysregulation resulted in demyelination; this finding identifies a signaling pathway that induces myelin breakdown in vivo. These findings are relevant for understanding the molecular mechanisms that control Schwann cell plasticity and underlie nerve pathology, including demyelinating neuropathies and tumorigenesis.

Original language	Undefined/Unknown
Pages (from-to)	839-U46
Journal	Nature Neuroscience
Volume	12
Issue number	7
DOIs	https://doi.org/10.1038/nn.2323
Publication status	Published - 2009

Access to Document

10.1038/nn.2323

http://hdl.handle.net/1765/24586

Cite this

Woodhoo, A., Alonso, MBD., Droggiti, A., Turmaine, M., D'Antonio, M., Parkinson, DB., Wilton, DK., Al-Shawi, R., Simons, P., Shen, J., Guillemot, F., Radtke, F., Meijer, D., Feltri, ML., Wrabetz, L., Mirsky, R., & Jessen, KR. (2009). Notch controls embryonic Schwann cell differentiation, postnatal myelination and adult plasticity. Nature Neuroscience, 12(7), 839-U46. https://doi.org/10.1038/nn.2323

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title = "Notch controls embryonic Schwann cell differentiation, postnatal myelination and adult plasticity",

abstract = "Notch signaling is central to vertebrate development, and analysis of Notch has provided important insights into pathogenetic mechanisms in the CNS and many other tissues. However, surprisingly little is known about the role of Notch in the development and pathology of Schwann cells and peripheral nerves. Using transgenic mice and cell cultures, we found that Notch has complex and extensive regulatory functions in Schwann cells. Notch promoted the generation of Schwann cells from Schwann cell precursors and regulated the size of the Schwann cell pool by controlling proliferation. Notch inhibited myelination, establishing that myelination is subject to negative transcriptional regulation that opposes forward drives such as Krox20. Notably, in the adult, Notch dysregulation resulted in demyelination; this finding identifies a signaling pathway that induces myelin breakdown in vivo. These findings are relevant for understanding the molecular mechanisms that control Schwann cell plasticity and underlie nerve pathology, including demyelinating neuropathies and tumorigenesis.",

author = "A Woodhoo and MBD Alonso and A Droggiti and M Turmaine and M D'Antonio and DB Parkinson and DK Wilton and R Al-Shawi and P Simons and J Shen and F Guillemot and F Radtke and Dies Meijer and ML Feltri and L Wrabetz and R Mirsky and KR Jessen",

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Woodhoo, A, Alonso, MBD, Droggiti, A, Turmaine, M, D'Antonio, M, Parkinson, DB, Wilton, DK, Al-Shawi, R, Simons, P, Shen, J, Guillemot, F, Radtke, F, Meijer, D, Feltri, ML, Wrabetz, L, Mirsky, R & Jessen, KR 2009, 'Notch controls embryonic Schwann cell differentiation, postnatal myelination and adult plasticity', Nature Neuroscience, vol. 12, no. 7, pp. 839-U46. https://doi.org/10.1038/nn.2323

TY - JOUR

T1 - Notch controls embryonic Schwann cell differentiation, postnatal myelination and adult plasticity

AU - Woodhoo, A

AU - Alonso, MBD

AU - Droggiti, A

AU - Turmaine, M

AU - D'Antonio, M

AU - Parkinson, DB

AU - Wilton, DK

AU - Al-Shawi, R

AU - Simons, P

AU - Shen, J

AU - Guillemot, F

AU - Radtke, F

AU - Meijer, Dies

AU - Feltri, ML

AU - Wrabetz, L

AU - Mirsky, R

AU - Jessen, KR

PY - 2009

Y1 - 2009

N2 - Notch signaling is central to vertebrate development, and analysis of Notch has provided important insights into pathogenetic mechanisms in the CNS and many other tissues. However, surprisingly little is known about the role of Notch in the development and pathology of Schwann cells and peripheral nerves. Using transgenic mice and cell cultures, we found that Notch has complex and extensive regulatory functions in Schwann cells. Notch promoted the generation of Schwann cells from Schwann cell precursors and regulated the size of the Schwann cell pool by controlling proliferation. Notch inhibited myelination, establishing that myelination is subject to negative transcriptional regulation that opposes forward drives such as Krox20. Notably, in the adult, Notch dysregulation resulted in demyelination; this finding identifies a signaling pathway that induces myelin breakdown in vivo. These findings are relevant for understanding the molecular mechanisms that control Schwann cell plasticity and underlie nerve pathology, including demyelinating neuropathies and tumorigenesis.

AB - Notch signaling is central to vertebrate development, and analysis of Notch has provided important insights into pathogenetic mechanisms in the CNS and many other tissues. However, surprisingly little is known about the role of Notch in the development and pathology of Schwann cells and peripheral nerves. Using transgenic mice and cell cultures, we found that Notch has complex and extensive regulatory functions in Schwann cells. Notch promoted the generation of Schwann cells from Schwann cell precursors and regulated the size of the Schwann cell pool by controlling proliferation. Notch inhibited myelination, establishing that myelination is subject to negative transcriptional regulation that opposes forward drives such as Krox20. Notably, in the adult, Notch dysregulation resulted in demyelination; this finding identifies a signaling pathway that induces myelin breakdown in vivo. These findings are relevant for understanding the molecular mechanisms that control Schwann cell plasticity and underlie nerve pathology, including demyelinating neuropathies and tumorigenesis.

U2 - 10.1038/nn.2323

DO - 10.1038/nn.2323

M3 - Article

SN - 1097-6256

VL - 12

SP - 839-U46

JO - Nature Neuroscience

JF - Nature Neuroscience

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