P2X4 receptor controls microglia activation and favors remyelination in autoimmune encephalitis

Microglia survey the brain microenvironment for signals of injury or infection and are essential for the initiation and resolution of pathogen‐ or tissue damage‐induced inflammation. Understanding the mechanism of microglia responses during pathology is hence vital to promote regenerative responses....

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Autores principales: Zabala, Alazne, Vazquez‐Villoldo, Nuria, Rissiek, Björn, Gejo, Jon, Martin, Abraham, Palomino, Aitor, Perez‐Samartín, Alberto, Pulagam, Krishna R, Lukowiak, Marco, Capetillo‐Zarate, Estibaliz, Llop, Jordi, Magnus, Tim, Koch‐Nolte, Friedrich, Rassendren, Francois, Matute, Carlos, Domercq, María
Formato: Online Artículo Texto
Lenguaje:English
Publicado: John Wiley and Sons Inc. 2018
Materias:
Research Articles
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6079537/
https://www.ncbi.nlm.nih.gov/pubmed/29973381
http://dx.doi.org/10.15252/emmm.201708743
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author Zabala, Alazne
Vazquez‐Villoldo, Nuria
Rissiek, Björn
Gejo, Jon
Martin, Abraham
Palomino, Aitor
Perez‐Samartín, Alberto
Pulagam, Krishna R
Lukowiak, Marco
Capetillo‐Zarate, Estibaliz
Llop, Jordi
Magnus, Tim
Koch‐Nolte, Friedrich
Rassendren, Francois
Matute, Carlos
Domercq, María
author_facet Zabala, Alazne
Vazquez‐Villoldo, Nuria
Rissiek, Björn
Gejo, Jon
Martin, Abraham
Palomino, Aitor
Perez‐Samartín, Alberto
Pulagam, Krishna R
Lukowiak, Marco
Capetillo‐Zarate, Estibaliz
Llop, Jordi
Magnus, Tim
Koch‐Nolte, Friedrich
Rassendren, Francois
Matute, Carlos
Domercq, María
author_sort Zabala, Alazne
collection PubMed
description Microglia survey the brain microenvironment for signals of injury or infection and are essential for the initiation and resolution of pathogen‐ or tissue damage‐induced inflammation. Understanding the mechanism of microglia responses during pathology is hence vital to promote regenerative responses. Here, we analyzed the role of purinergic receptor P2X4 (P2X4R) in microglia/macrophages during autoimmune inflammation. Blockade of P2X4R signaling exacerbated clinical signs in the experimental autoimmune encephalomyelitis (EAE) model and also favored microglia activation to a pro‐inflammatory phenotype and inhibited myelin phagocytosis. Moreover, P2X4R blockade in microglia halted oligodendrocyte differentiation in vitro and remyelination after lysolecithin‐induced demyelination. Conversely, potentiation of P2X4R signaling by the allosteric modulator ivermectin (IVM) favored a switch in microglia to an anti‐inflammatory phenotype, potentiated myelin phagocytosis, promoted the remyelination response, and ameliorated clinical signs of EAE. Our results provide evidence that P2X4Rs modulate microglia/macrophage inflammatory responses and identify IVM as a potential candidate among currently used drugs to promote the repair of myelin damage.
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spelling pubmed-60795372018-08-09 P2X4 receptor controls microglia activation and favors remyelination in autoimmune encephalitis Zabala, Alazne Vazquez‐Villoldo, Nuria Rissiek, Björn Gejo, Jon Martin, Abraham Palomino, Aitor Perez‐Samartín, Alberto Pulagam, Krishna R Lukowiak, Marco Capetillo‐Zarate, Estibaliz Llop, Jordi Magnus, Tim Koch‐Nolte, Friedrich Rassendren, Francois Matute, Carlos Domercq, María EMBO Mol Med Research Articles Microglia survey the brain microenvironment for signals of injury or infection and are essential for the initiation and resolution of pathogen‐ or tissue damage‐induced inflammation. Understanding the mechanism of microglia responses during pathology is hence vital to promote regenerative responses. Here, we analyzed the role of purinergic receptor P2X4 (P2X4R) in microglia/macrophages during autoimmune inflammation. Blockade of P2X4R signaling exacerbated clinical signs in the experimental autoimmune encephalomyelitis (EAE) model and also favored microglia activation to a pro‐inflammatory phenotype and inhibited myelin phagocytosis. Moreover, P2X4R blockade in microglia halted oligodendrocyte differentiation in vitro and remyelination after lysolecithin‐induced demyelination. Conversely, potentiation of P2X4R signaling by the allosteric modulator ivermectin (IVM) favored a switch in microglia to an anti‐inflammatory phenotype, potentiated myelin phagocytosis, promoted the remyelination response, and ameliorated clinical signs of EAE. Our results provide evidence that P2X4Rs modulate microglia/macrophage inflammatory responses and identify IVM as a potential candidate among currently used drugs to promote the repair of myelin damage. John Wiley and Sons Inc. 2018-07-04 2018-08 /pmc/articles/PMC6079537/ /pubmed/29973381 http://dx.doi.org/10.15252/emmm.201708743 Text en © 2018 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 Research Articles
Zabala, Alazne
Vazquez‐Villoldo, Nuria
Rissiek, Björn
Gejo, Jon
Martin, Abraham
Palomino, Aitor
Perez‐Samartín, Alberto
Pulagam, Krishna R
Lukowiak, Marco
Capetillo‐Zarate, Estibaliz
Llop, Jordi
Magnus, Tim
Koch‐Nolte, Friedrich
Rassendren, Francois
Matute, Carlos
Domercq, María
P2X4 receptor controls microglia activation and favors remyelination in autoimmune encephalitis
title P2X4 receptor controls microglia activation and favors remyelination in autoimmune encephalitis
title_full P2X4 receptor controls microglia activation and favors remyelination in autoimmune encephalitis
title_fullStr P2X4 receptor controls microglia activation and favors remyelination in autoimmune encephalitis
title_full_unstemmed P2X4 receptor controls microglia activation and favors remyelination in autoimmune encephalitis
title_short P2X4 receptor controls microglia activation and favors remyelination in autoimmune encephalitis
title_sort p2x4 receptor controls microglia activation and favors remyelination in autoimmune encephalitis
topic Research Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6079537/
https://www.ncbi.nlm.nih.gov/pubmed/29973381
http://dx.doi.org/10.15252/emmm.201708743
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