Disruption of Sema3A/Plexin‐A1 inhibitory signalling in oligodendrocytes as a therapeutic strategy to promote remyelination

Current treatments in multiple sclerosis (MS) are modulating the inflammatory component of the disease, but no drugs are currently available to repair lesions. Our study identifies in MS patients the overexpression of Plexin‐A1, the signalling receptor of the oligodendrocyte inhibitor Semaphorin 3A....

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Autores principales: Binamé, Fabien, Pham‐Van, Lucas D, Spenlé, Caroline, Jolivel, Valérie, Birmpili, Dafni, Meyer, Lionel A, Jacob, Laurent, Meyer, Laurence, Mensah‐Nyagan, Ayikoé G, Po, Chrystelle, Van der Heyden, Michaël, Roussel, Guy, Bagnard, Dominique
Formato: Online Artículo Texto
Lenguaje:English
Publicado: John Wiley and Sons Inc. 2019
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Articles
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6835579/
https://www.ncbi.nlm.nih.gov/pubmed/31566924
http://dx.doi.org/10.15252/emmm.201910378
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author Binamé, Fabien
Pham‐Van, Lucas D
Spenlé, Caroline
Jolivel, Valérie
Birmpili, Dafni
Meyer, Lionel A
Jacob, Laurent
Meyer, Laurence
Mensah‐Nyagan, Ayikoé G
Po, Chrystelle
Van der Heyden, Michaël
Roussel, Guy
Bagnard, Dominique
author_facet Binamé, Fabien
Pham‐Van, Lucas D
Spenlé, Caroline
Jolivel, Valérie
Birmpili, Dafni
Meyer, Lionel A
Jacob, Laurent
Meyer, Laurence
Mensah‐Nyagan, Ayikoé G
Po, Chrystelle
Van der Heyden, Michaël
Roussel, Guy
Bagnard, Dominique
author_sort Binamé, Fabien
collection PubMed
description Current treatments in multiple sclerosis (MS) are modulating the inflammatory component of the disease, but no drugs are currently available to repair lesions. Our study identifies in MS patients the overexpression of Plexin‐A1, the signalling receptor of the oligodendrocyte inhibitor Semaphorin 3A. Using a novel type of peptidic antagonist, we showed the possibility to counteract the Sema3A inhibitory effect on oligodendrocyte migration and differentiation in vitro when antagonizing Plexin‐A1. The use of this compound in vivo demonstrated a myelin protective effect as shown with DTI‐MRI and confirmed at the histological level in the mouse cuprizone model of induced demyelination/remyelination. This effect correlated with locomotor performances fully preserved in chronically treated animals. The administration of the peptide also showed protective effects, leading to a reduced severity of demyelination in the context of experimental autoimmune encephalitis (EAE). Hence, the disruption of the inhibitory microenvironmental molecular barriers allows normal myelinating cells to exert their spontaneous remyelinating capacity. This opens unprecedented therapeutic opportunity for patients suffering a disease for which no curative options are yet available.
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spelling pubmed-68355792019-11-08 Disruption of Sema3A/Plexin‐A1 inhibitory signalling in oligodendrocytes as a therapeutic strategy to promote remyelination Binamé, Fabien Pham‐Van, Lucas D Spenlé, Caroline Jolivel, Valérie Birmpili, Dafni Meyer, Lionel A Jacob, Laurent Meyer, Laurence Mensah‐Nyagan, Ayikoé G Po, Chrystelle Van der Heyden, Michaël Roussel, Guy Bagnard, Dominique EMBO Mol Med Articles Current treatments in multiple sclerosis (MS) are modulating the inflammatory component of the disease, but no drugs are currently available to repair lesions. Our study identifies in MS patients the overexpression of Plexin‐A1, the signalling receptor of the oligodendrocyte inhibitor Semaphorin 3A. Using a novel type of peptidic antagonist, we showed the possibility to counteract the Sema3A inhibitory effect on oligodendrocyte migration and differentiation in vitro when antagonizing Plexin‐A1. The use of this compound in vivo demonstrated a myelin protective effect as shown with DTI‐MRI and confirmed at the histological level in the mouse cuprizone model of induced demyelination/remyelination. This effect correlated with locomotor performances fully preserved in chronically treated animals. The administration of the peptide also showed protective effects, leading to a reduced severity of demyelination in the context of experimental autoimmune encephalitis (EAE). Hence, the disruption of the inhibitory microenvironmental molecular barriers allows normal myelinating cells to exert their spontaneous remyelinating capacity. This opens unprecedented therapeutic opportunity for patients suffering a disease for which no curative options are yet available. John Wiley and Sons Inc. 2019-09-30 2019-11-07 /pmc/articles/PMC6835579/ /pubmed/31566924 http://dx.doi.org/10.15252/emmm.201910378 Text en © 2019 The Authors. Published under the terms of the CC BY 4.0 license This is an open access article under the terms of the http://creativecommons.org/licenses/by/4.0/ License, which permits use, distribution and reproduction in any medium, provided the original work is properly cited.
spellingShingle Articles
Binamé, Fabien
Pham‐Van, Lucas D
Spenlé, Caroline
Jolivel, Valérie
Birmpili, Dafni
Meyer, Lionel A
Jacob, Laurent
Meyer, Laurence
Mensah‐Nyagan, Ayikoé G
Po, Chrystelle
Van der Heyden, Michaël
Roussel, Guy
Bagnard, Dominique
Disruption of Sema3A/Plexin‐A1 inhibitory signalling in oligodendrocytes as a therapeutic strategy to promote remyelination
title Disruption of Sema3A/Plexin‐A1 inhibitory signalling in oligodendrocytes as a therapeutic strategy to promote remyelination
title_full Disruption of Sema3A/Plexin‐A1 inhibitory signalling in oligodendrocytes as a therapeutic strategy to promote remyelination
title_fullStr Disruption of Sema3A/Plexin‐A1 inhibitory signalling in oligodendrocytes as a therapeutic strategy to promote remyelination
title_full_unstemmed Disruption of Sema3A/Plexin‐A1 inhibitory signalling in oligodendrocytes as a therapeutic strategy to promote remyelination
title_short Disruption of Sema3A/Plexin‐A1 inhibitory signalling in oligodendrocytes as a therapeutic strategy to promote remyelination
title_sort disruption of sema3a/plexin‐a1 inhibitory signalling in oligodendrocytes as a therapeutic strategy to promote remyelination
topic Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6835579/
https://www.ncbi.nlm.nih.gov/pubmed/31566924
http://dx.doi.org/10.15252/emmm.201910378
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