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Literature DB >> 29610440

Sustained Expression of Negative Regulators of Myelination Protects Schwann Cells from Dysmyelination in a Charcot-Marie-Tooth 1B Mouse Model.

Francesca Florio¹, Cinzia Ferri¹, Cristina Scapin¹, M Laura Feltri^2,3,4, Lawrence Wrabetz^2,3,4, Maurizio D'Antonio⁵.

Abstract

Schwann cell differentiation and myelination in the PNS are the result of fine-tuning of positive and negative transcriptional regulators. As myelination starts, negative regulators are downregulated, whereas positive ones are upregulated. Fully differentiated Schwann cells maintain an extraordinary plasticity and can transdifferentiate into "repair" Schwann cells after nerve injury. Reactivation of negative regulators of myelination is essential to generate repair Schwann cells. Negative regulators have also been implicated in demyelinating neuropathies, although their role in disease remains elusive. Here, we used a mouse model of Charcot-Marie-Tooth neuropathy type 1B (CMT1B), the P0S63del mouse characterized by ER stress and the activation of the unfolded protein response, to show that adult Schwann cells are in a partial differentiation state because they overexpress transcription factors that are normally expressed only before myelination. We provide evidence that two of these factors, Sox2 and Id2, act as negative regulators of myelination in vivo However, their sustained expression in neuropathy is protective because ablation of Sox2 or/and Id2 from S63del mice of both sexes results in worsening of the dysmyelinating phenotype. This is accompanied by increased levels of mutant P0 expression and exacerbation of ER stress, suggesting that limited differentiation may represent a novel adaptive mechanism through which Schwann cells counter the toxic effect of a mutant terminal differentiation protein.SIGNIFICANCE STATEMENT In many neuropathies, Schwann cells express high levels of early differentiation genes, but the significance of these altered expression remained unclear. Because many of these factors may act as negative regulators of myelination, it was suggested that their misexpression could contribute to dysmyelination. Here, we show that the transcription factors Sox2 and Id2 act as negative regulators of myelination in vivo, but that their sustained expression in Charcot-Marie-Tooth type 1B (CMT1B) represents an adaptive response activated by the Schwann cells to reduce mutant protein toxicity and prevent demyelination.

Entities: CellLine Disease Gene Mutation Species

Keywords: Charcot–Marie–Tooth; Id2; Schwann cell; Sox2; UPR; myelin

Mesh：

Substances：

Year: 2018 PMID： 29610440 PMCID： PMC6596005 DOI： 10.1523/JNEUROSCI.0201-18.2018

Source DB: PubMed Journal: J Neurosci ISSN： 0270-6474 Impact factor: 6.167

53 in total

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3. Helix-loop-helix proteins in Schwann cells: a study of regulation and subcellular localization of Ids, REB, and E12/47 during embryonic and postnatal development.

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4. MpzR98C arrests Schwann cell development in a mouse model of early-onset Charcot-Marie-Tooth disease type 1B.

Authors: Mario A C Saporta; Brian R Shy; Agnes Patzko; Yunhong Bai; Maria Pennuto; Cinzia Ferri; Elisa Tinelli; Paola Saveri; Dan Kirschner; Michelle Crowther; Cherie Southwood; Xingyao Wu; Alexander Gow; M Laura Feltri; Lawrence Wrabetz; Michael E Shy
Journal: Brain Date: 2012-06-10 Impact factor: 13.501

5. Analysis of congenital hypomyelinating Egr2Lo/Lo nerves identifies Sox2 as an inhibitor of Schwann cell differentiation and myelination.

Authors: Nam Le; Rakesh Nagarajan; James Y T Wang; Toshiyuki Araki; Robert E Schmidt; Jeffrey Milbrandt
Journal: Proc Natl Acad Sci U S A Date: 2005-02-03 Impact factor: 11.205

6. Clinical phenotypes of different MPZ (P0) mutations may include Charcot-Marie-Tooth type 1B, Dejerine-Sottas, and congenital hypomyelination.

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Journal: Neuron Date: 1996-09 Impact factor: 17.173

7. Identical point mutations of PMP-22 in Trembler-J mouse and Charcot-Marie-Tooth disease type 1A.

Authors: L J Valentijn; F Baas; R A Wolterman; J E Hoogendijk; N H van den Bosch; I Zorn; A W Gabreëls-Festen; M de Visser; P A Bolhuis
Journal: Nat Genet Date: 1992-12 Impact factor: 38.330

Review 8. The molecular machinery of myelin gene transcription in Schwann cells.

Authors: John Svaren; Dies Meijer
Journal: Glia Date: 2008-11-01 Impact factor: 8.073

Review 9. The repair Schwann cell and its function in regenerating nerves.

Authors: K R Jessen; R Mirsky
Journal: J Physiol Date: 2016-03-21 Impact factor: 5.182

10. Krox-20 inhibits Jun-NH2-terminal kinase/c-Jun to control Schwann cell proliferation and death.

Authors: David B Parkinson; Ambily Bhaskaran; Anna Droggiti; Sarah Dickinson; Maurizio D'Antonio; Rhona Mirsky; Kristjan R Jessen
Journal: J Cell Biol Date: 2004-02-02 Impact factor: 10.539

8 in total

1. Enhanced axonal neuregulin-1 type-III signaling ameliorates neurophysiology and hypomyelination in a Charcot-Marie-Tooth type 1B mouse model.

Authors: Cristina Scapin; Cinzia Ferri; Emanuela Pettinato; Desiree Zambroni; Francesca Bianchi; Ubaldo Del Carro; Sophie Belin; Donatella Caruso; Nico Mitro; Marta Pellegatta; Carla Taveggia; Markus H Schwab; Klaus-Armin Nave; M Laura Feltri; Lawrence Wrabetz; Maurizio D'Antonio
Journal: Hum Mol Genet Date: 2019-03-15 Impact factor: 6.150

2. Phosphorylation of eIF2α Promotes Schwann Cell Differentiation and Myelination in CMT1B Mice with Activated UPR.

Authors: Cristina Scapin; Cinzia Ferri; Emanuela Pettinato; Francesca Bianchi; Ubaldo Del Carro; M Laura Feltri; Randal J Kaufman; Lawrence Wrabetz; Maurizio D'Antonio
Journal: J Neurosci Date: 2020-09-24 Impact factor: 6.167

Review 3. Lessons from Injury: How Nerve Injury Studies Reveal Basic Biological Mechanisms and Therapeutic Opportunities for Peripheral Nerve Diseases.

Authors: Peter Arthur-Farraj; Michael P Coleman
Journal: Neurotherapeutics Date: 2021-09-30 Impact factor: 7.620

Review 4. The Role of c-Jun and Autocrine Signaling Loops in the Control of Repair Schwann Cells and Regeneration.

Authors: Kristjan R Jessen; Rhona Mirsky
Journal: Front Cell Neurosci Date: 2022-02-09 Impact factor: 5.505

5. Treatment with IFB-088 Improves Neuropathy in CMT1A and CMT1B Mice.

Authors: Michael E Shy; Maurizio D'Antonio; Yunhong Bai; Caroline Treins; Vera G Volpi; Cristina Scapin; Cinzia Ferri; Rosa Mastrangelo; Thierry Touvier; Francesca Florio; Francesca Bianchi; Ubaldo Del Carro; Frank F Baas; David Wang; Pierre Miniou; Philippe Guedat
Journal: Mol Neurobiol Date: 2022-04-30 Impact factor: 5.682