Development of NMDAR Antagonists with Reduced Neurotoxic Side Effects: a Study on GK11

The NMDAR glutamate receptor subtype mediates various vital physiological neuronal functions. However, its excessive activation contributes to neuronal damage in a large variety of acute and chronic neurological disorders. NMDAR antagonists thus represent promising therapeutic tools that can counter...

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Autores principales: Vandame, Delphine, Ulmann, Lauriane, Teigell, Marisa, Prieto-Cappellini, Monica, Vignon, Jacques, Privat, Alain, Perez-Polo, Regino, Nesic, Olivera, Hirbec, Helene
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2013
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3834252/
https://www.ncbi.nlm.nih.gov/pubmed/24260528
http://dx.doi.org/10.1371/journal.pone.0081004
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author Vandame, Delphine
Ulmann, Lauriane
Teigell, Marisa
Prieto-Cappellini, Monica
Vignon, Jacques
Privat, Alain
Perez-Polo, Regino
Nesic, Olivera
Hirbec, Helene
author_facet Vandame, Delphine
Ulmann, Lauriane
Teigell, Marisa
Prieto-Cappellini, Monica
Vignon, Jacques
Privat, Alain
Perez-Polo, Regino
Nesic, Olivera
Hirbec, Helene
author_sort Vandame, Delphine
collection PubMed
description The NMDAR glutamate receptor subtype mediates various vital physiological neuronal functions. However, its excessive activation contributes to neuronal damage in a large variety of acute and chronic neurological disorders. NMDAR antagonists thus represent promising therapeutic tools that can counteract NMDARs’ overactivation. Channel blockers are of special interest since they are use-dependent, thus being more potent at continuously activated NMDARs, as may be the case in pathological conditions. Nevertheless, it has been established that NMDAR antagonists, such as MK801, also have unacceptable neurotoxic effects. Presently only Memantine is considered a safe NMDAR antagonist and is used clinically. It has recently been speculated that antagonists that preferentially target extrasynaptic NMDARs would be less toxic. We previously demonstrated that the phencyclidine derivative GK11 preferentially inhibits extrasynaptic NMDARs. We thus anticipated that this compound would be safer than other known NMDAR antagonists. In this study we used whole-genome profiling of the rat cingulate cortex, a brain area that is particularly sensitive to NMDAR antagonists, to compare the potential adverse effects of GK11 and MK801. Our results showed that in contrast to GK11, the transcriptional profile of MK801 is characterized by a significant upregulation of inflammatory and stress-response genes, consistent with its high neurotoxicity. In addition, behavioural and immunohistochemical analyses confirmed marked inflammatory reactions (including astrogliosis and microglial activation) in MK801-treated, but not GK11-treated rats. Interestingly, we also showed that GK11 elicited less inflammation and neuronal damage, even when compared to Memantine, which like GK11, preferentially inhibits extrasynaptic NMDAR. As a whole, our study suggests that GK11 may be a more attractive therapeutic alternative in the treatment of CNS disorders characterized by the overactivation of glutamate receptors.
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spelling pubmed-38342522013-11-20 Development of NMDAR Antagonists with Reduced Neurotoxic Side Effects: a Study on GK11 Vandame, Delphine Ulmann, Lauriane Teigell, Marisa Prieto-Cappellini, Monica Vignon, Jacques Privat, Alain Perez-Polo, Regino Nesic, Olivera Hirbec, Helene PLoS One Research Article The NMDAR glutamate receptor subtype mediates various vital physiological neuronal functions. However, its excessive activation contributes to neuronal damage in a large variety of acute and chronic neurological disorders. NMDAR antagonists thus represent promising therapeutic tools that can counteract NMDARs’ overactivation. Channel blockers are of special interest since they are use-dependent, thus being more potent at continuously activated NMDARs, as may be the case in pathological conditions. Nevertheless, it has been established that NMDAR antagonists, such as MK801, also have unacceptable neurotoxic effects. Presently only Memantine is considered a safe NMDAR antagonist and is used clinically. It has recently been speculated that antagonists that preferentially target extrasynaptic NMDARs would be less toxic. We previously demonstrated that the phencyclidine derivative GK11 preferentially inhibits extrasynaptic NMDARs. We thus anticipated that this compound would be safer than other known NMDAR antagonists. In this study we used whole-genome profiling of the rat cingulate cortex, a brain area that is particularly sensitive to NMDAR antagonists, to compare the potential adverse effects of GK11 and MK801. Our results showed that in contrast to GK11, the transcriptional profile of MK801 is characterized by a significant upregulation of inflammatory and stress-response genes, consistent with its high neurotoxicity. In addition, behavioural and immunohistochemical analyses confirmed marked inflammatory reactions (including astrogliosis and microglial activation) in MK801-treated, but not GK11-treated rats. Interestingly, we also showed that GK11 elicited less inflammation and neuronal damage, even when compared to Memantine, which like GK11, preferentially inhibits extrasynaptic NMDAR. As a whole, our study suggests that GK11 may be a more attractive therapeutic alternative in the treatment of CNS disorders characterized by the overactivation of glutamate receptors. Public Library of Science 2013-11-19 /pmc/articles/PMC3834252/ /pubmed/24260528 http://dx.doi.org/10.1371/journal.pone.0081004 Text en https://creativecommons.org/publicdomain/zero/1.0/ This is an open-access article distributed under the terms of the Creative Commons Public Domain declaration, which stipulates that, once placed in the public domain, this work may be freely reproduced, distributed, transmitted, modified, built upon, or otherwise used by anyone for any lawful purpose.
spellingShingle Research Article
Vandame, Delphine
Ulmann, Lauriane
Teigell, Marisa
Prieto-Cappellini, Monica
Vignon, Jacques
Privat, Alain
Perez-Polo, Regino
Nesic, Olivera
Hirbec, Helene
Development of NMDAR Antagonists with Reduced Neurotoxic Side Effects: a Study on GK11
title Development of NMDAR Antagonists with Reduced Neurotoxic Side Effects: a Study on GK11
title_full Development of NMDAR Antagonists with Reduced Neurotoxic Side Effects: a Study on GK11
title_fullStr Development of NMDAR Antagonists with Reduced Neurotoxic Side Effects: a Study on GK11
title_full_unstemmed Development of NMDAR Antagonists with Reduced Neurotoxic Side Effects: a Study on GK11
title_short Development of NMDAR Antagonists with Reduced Neurotoxic Side Effects: a Study on GK11
title_sort development of nmdar antagonists with reduced neurotoxic side effects: a study on gk11
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3834252/
https://www.ncbi.nlm.nih.gov/pubmed/24260528
http://dx.doi.org/10.1371/journal.pone.0081004
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