Characterization of phenotype markers and neuronotoxic potential of polarised primary microglia in vitro

Microglia mediate multiple facets of neuroinflammation, including cytotoxicity, repair, regeneration, and immunosuppression due to their ability to acquire diverse activation states, or phenotypes. Modulation of microglial phenotype is an appealing neurotherapeutic strategy but a comprehensive study...

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Autores principales: Chhor, Vibol, Le Charpentier, Tifenn, Lebon, Sophie, Oré, Marie-Virgine, Celador, Idoia Lara, Josserand, Julien, Degos, Vincent, Jacotot, Etienne, Hagberg, Henrik, Sävman, Karin, Mallard, Carina, Gressens, Pierre, Fleiss, Bobbi
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Academic Press 2013
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3694309/
https://www.ncbi.nlm.nih.gov/pubmed/23454862
http://dx.doi.org/10.1016/j.bbi.2013.02.005
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author Chhor, Vibol
Le Charpentier, Tifenn
Lebon, Sophie
Oré, Marie-Virgine
Celador, Idoia Lara
Josserand, Julien
Degos, Vincent
Jacotot, Etienne
Hagberg, Henrik
Sävman, Karin
Mallard, Carina
Gressens, Pierre
Fleiss, Bobbi
author_facet Chhor, Vibol
Le Charpentier, Tifenn
Lebon, Sophie
Oré, Marie-Virgine
Celador, Idoia Lara
Josserand, Julien
Degos, Vincent
Jacotot, Etienne
Hagberg, Henrik
Sävman, Karin
Mallard, Carina
Gressens, Pierre
Fleiss, Bobbi
author_sort Chhor, Vibol
collection PubMed
description Microglia mediate multiple facets of neuroinflammation, including cytotoxicity, repair, regeneration, and immunosuppression due to their ability to acquire diverse activation states, or phenotypes. Modulation of microglial phenotype is an appealing neurotherapeutic strategy but a comprehensive study of classical and more novel microglial phenotypic markers in vitro is lacking. The aim of this study was to outline the temporal expression of a battery of phenotype markers from polarised microglia to generate an in vitro tool for screening the immunomodulatory potential of novel compounds. We characterised expression of thirty-one macrophage/microglial phenotype markers in primary microglia over time (4, 12, 36, and 72 h), using RT-qPCR or multiplex protein assay. Firstly, we selected Interleukin-4 (IL-4) and lipopolysaccharide (LPS) as the strongest M1–M2 polarising stimuli, from six stimuli tested. At each time point, markers useful to identify that microglia were M1 included iNOS, Cox-2 and IL-6 and a loss of M2a markers. Markers useful for quantifying M2b-immunomodulatory microglia included, increased IL-1RA and SOCS3 and for M2a-repair and regeneration, included increased arginase-1, and a loss of the M1 and M2b markers were discriminatory. Additional markers were regulated at fewer time points, but are still likely important to monitor when assessing the immunomodulatory potential of novel therapies. Further, to facilitate identification of how novel immunomodulatory treatments alter the functional affects of microglia, we characterised how the soluble products from polarised microglia affected the type and rate of neuronal death; M1/2b induced increasing and M2a-induced decreasing neuronal loss. We also assessed any effects of prior activation state, to provide a way to identify how a novel compound may alter phenotype depending on the stage of injury/insult progression. We identified generally that a prior M1/2b reduced the ability of microglia to switch to M2a. Altogether, we have characterised a profile of phenotype markers and a mechanism of assessing functional outcome that we can use as a reference guide for first-line screening of novel immunomodulatory therapies in vitro in the search for viable neuroprotectants.
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spelling pubmed-36943092013-08-01 Characterization of phenotype markers and neuronotoxic potential of polarised primary microglia in vitro Chhor, Vibol Le Charpentier, Tifenn Lebon, Sophie Oré, Marie-Virgine Celador, Idoia Lara Josserand, Julien Degos, Vincent Jacotot, Etienne Hagberg, Henrik Sävman, Karin Mallard, Carina Gressens, Pierre Fleiss, Bobbi Brain Behav Immun Article Microglia mediate multiple facets of neuroinflammation, including cytotoxicity, repair, regeneration, and immunosuppression due to their ability to acquire diverse activation states, or phenotypes. Modulation of microglial phenotype is an appealing neurotherapeutic strategy but a comprehensive study of classical and more novel microglial phenotypic markers in vitro is lacking. The aim of this study was to outline the temporal expression of a battery of phenotype markers from polarised microglia to generate an in vitro tool for screening the immunomodulatory potential of novel compounds. We characterised expression of thirty-one macrophage/microglial phenotype markers in primary microglia over time (4, 12, 36, and 72 h), using RT-qPCR or multiplex protein assay. Firstly, we selected Interleukin-4 (IL-4) and lipopolysaccharide (LPS) as the strongest M1–M2 polarising stimuli, from six stimuli tested. At each time point, markers useful to identify that microglia were M1 included iNOS, Cox-2 and IL-6 and a loss of M2a markers. Markers useful for quantifying M2b-immunomodulatory microglia included, increased IL-1RA and SOCS3 and for M2a-repair and regeneration, included increased arginase-1, and a loss of the M1 and M2b markers were discriminatory. Additional markers were regulated at fewer time points, but are still likely important to monitor when assessing the immunomodulatory potential of novel therapies. Further, to facilitate identification of how novel immunomodulatory treatments alter the functional affects of microglia, we characterised how the soluble products from polarised microglia affected the type and rate of neuronal death; M1/2b induced increasing and M2a-induced decreasing neuronal loss. We also assessed any effects of prior activation state, to provide a way to identify how a novel compound may alter phenotype depending on the stage of injury/insult progression. We identified generally that a prior M1/2b reduced the ability of microglia to switch to M2a. Altogether, we have characterised a profile of phenotype markers and a mechanism of assessing functional outcome that we can use as a reference guide for first-line screening of novel immunomodulatory therapies in vitro in the search for viable neuroprotectants. Academic Press 2013-08 /pmc/articles/PMC3694309/ /pubmed/23454862 http://dx.doi.org/10.1016/j.bbi.2013.02.005 Text en © 2013 Elsevier Inc. https://creativecommons.org/licenses/by/3.0/ Open Access under CC BY 3.0 (https://creativecommons.org/licenses/by/3.0/) license
spellingShingle Article
Chhor, Vibol
Le Charpentier, Tifenn
Lebon, Sophie
Oré, Marie-Virgine
Celador, Idoia Lara
Josserand, Julien
Degos, Vincent
Jacotot, Etienne
Hagberg, Henrik
Sävman, Karin
Mallard, Carina
Gressens, Pierre
Fleiss, Bobbi
Characterization of phenotype markers and neuronotoxic potential of polarised primary microglia in vitro
title Characterization of phenotype markers and neuronotoxic potential of polarised primary microglia in vitro
title_full Characterization of phenotype markers and neuronotoxic potential of polarised primary microglia in vitro
title_fullStr Characterization of phenotype markers and neuronotoxic potential of polarised primary microglia in vitro
title_full_unstemmed Characterization of phenotype markers and neuronotoxic potential of polarised primary microglia in vitro
title_short Characterization of phenotype markers and neuronotoxic potential of polarised primary microglia in vitro
title_sort characterization of phenotype markers and neuronotoxic potential of polarised primary microglia in vitro
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3694309/
https://www.ncbi.nlm.nih.gov/pubmed/23454862
http://dx.doi.org/10.1016/j.bbi.2013.02.005
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