Glutamate-induced and NMDA receptor-mediated neurodegeneration entails P2Y1 receptor activation

Despite the characteristic etiologies and phenotypes, different brain disorders rely on common pathogenic events. Glutamate-induced neurotoxicity is a pathogenic event shared by different brain disorders. Another event occurring in different brain pathological conditions is the increase of the extra...

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Autores principales: Simões, Ana P., Silva, Carla G., Marques, Joana M., Pochmann, Daniela, Porciúncula, Lisiane O., Ferreira, Sofia, Oses, Jean P., Beleza, Rui O., Real, Joana I., Köfalvi, Attila, Bahr, Ben A., Lerma, Juan, Cunha, Rodrigo A., Rodrigues, Ricardo J.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Nature Publishing Group UK 2018
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Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5833818/
https://www.ncbi.nlm.nih.gov/pubmed/29463792
http://dx.doi.org/10.1038/s41419-018-0351-1
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author Simões, Ana P.
Silva, Carla G.
Marques, Joana M.
Pochmann, Daniela
Porciúncula, Lisiane O.
Ferreira, Sofia
Oses, Jean P.
Beleza, Rui O.
Real, Joana I.
Köfalvi, Attila
Bahr, Ben A.
Lerma, Juan
Cunha, Rodrigo A.
Rodrigues, Ricardo J.
author_facet Simões, Ana P.
Silva, Carla G.
Marques, Joana M.
Pochmann, Daniela
Porciúncula, Lisiane O.
Ferreira, Sofia
Oses, Jean P.
Beleza, Rui O.
Real, Joana I.
Köfalvi, Attila
Bahr, Ben A.
Lerma, Juan
Cunha, Rodrigo A.
Rodrigues, Ricardo J.
author_sort Simões, Ana P.
collection PubMed
description Despite the characteristic etiologies and phenotypes, different brain disorders rely on common pathogenic events. Glutamate-induced neurotoxicity is a pathogenic event shared by different brain disorders. Another event occurring in different brain pathological conditions is the increase of the extracellular ATP levels, which is now recognized as a danger and harmful signal in the brain, as heralded by the ability of P2 receptors (P2Rs) to affect a wide range of brain disorders. Yet, how ATP and P2R contribute to neurodegeneration remains poorly defined. For that purpose, we now examined the contribution of extracellular ATP and P2Rs to glutamate-induced neurodegeneration. We found both in vitro and in vivo that ATP/ADP through the activation of P2Y1R contributes to glutamate-induced neuronal death in the rat hippocampus. We found in cultured rat hippocampal neurons that the exposure to glutamate (100 µM) for 30 min triggers a sustained increase of extracellular ATP levels, which contributes to NMDA receptor (NMDAR)-mediated hippocampal neuronal death through the activation of P2Y1R. We also determined that P2Y1R is involved in excitotoxicity in vivo as the blockade of P2Y1R significantly attenuated rat hippocampal neuronal death upon the systemic administration of kainic acid or upon the intrahippocampal injection of quinolinic acid. This contribution of P2Y1R fades with increasing intensity of excitotoxic conditions, which indicates that P2Y1R is not contributing directly to neurodegeneration, rather behaving as a catalyst decreasing the threshold from which glutamate becomes neurotoxic. Moreover, we unraveled that such excitotoxicity process began with an early synaptotoxicity that was also prevented/attenuated by the antagonism of P2Y1R, both in vitro and in vivo. This should rely on the observed glutamate-induced calpain-mediated axonal cytoskeleton damage, most likely favored by a P2Y1R-driven increase of NMDAR-mediated Ca(2+) entry selectively in axons. This may constitute a degenerative mechanism shared by different brain diseases, particularly relevant at initial pathogenic stages.
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spelling pubmed-58338182018-03-06 Glutamate-induced and NMDA receptor-mediated neurodegeneration entails P2Y1 receptor activation Simões, Ana P. Silva, Carla G. Marques, Joana M. Pochmann, Daniela Porciúncula, Lisiane O. Ferreira, Sofia Oses, Jean P. Beleza, Rui O. Real, Joana I. Köfalvi, Attila Bahr, Ben A. Lerma, Juan Cunha, Rodrigo A. Rodrigues, Ricardo J. Cell Death Dis Article Despite the characteristic etiologies and phenotypes, different brain disorders rely on common pathogenic events. Glutamate-induced neurotoxicity is a pathogenic event shared by different brain disorders. Another event occurring in different brain pathological conditions is the increase of the extracellular ATP levels, which is now recognized as a danger and harmful signal in the brain, as heralded by the ability of P2 receptors (P2Rs) to affect a wide range of brain disorders. Yet, how ATP and P2R contribute to neurodegeneration remains poorly defined. For that purpose, we now examined the contribution of extracellular ATP and P2Rs to glutamate-induced neurodegeneration. We found both in vitro and in vivo that ATP/ADP through the activation of P2Y1R contributes to glutamate-induced neuronal death in the rat hippocampus. We found in cultured rat hippocampal neurons that the exposure to glutamate (100 µM) for 30 min triggers a sustained increase of extracellular ATP levels, which contributes to NMDA receptor (NMDAR)-mediated hippocampal neuronal death through the activation of P2Y1R. We also determined that P2Y1R is involved in excitotoxicity in vivo as the blockade of P2Y1R significantly attenuated rat hippocampal neuronal death upon the systemic administration of kainic acid or upon the intrahippocampal injection of quinolinic acid. This contribution of P2Y1R fades with increasing intensity of excitotoxic conditions, which indicates that P2Y1R is not contributing directly to neurodegeneration, rather behaving as a catalyst decreasing the threshold from which glutamate becomes neurotoxic. Moreover, we unraveled that such excitotoxicity process began with an early synaptotoxicity that was also prevented/attenuated by the antagonism of P2Y1R, both in vitro and in vivo. This should rely on the observed glutamate-induced calpain-mediated axonal cytoskeleton damage, most likely favored by a P2Y1R-driven increase of NMDAR-mediated Ca(2+) entry selectively in axons. This may constitute a degenerative mechanism shared by different brain diseases, particularly relevant at initial pathogenic stages. Nature Publishing Group UK 2018-02-20 /pmc/articles/PMC5833818/ /pubmed/29463792 http://dx.doi.org/10.1038/s41419-018-0351-1 Text en © The Author(s) 2018 Open Access This article is licensed under a Creative Commons Attribution 4.0 International License, which permits use, sharing, adaptation, distribution and reproduction in any medium or format, as long as you give appropriate credit to the original author(s) and the source, provide a link to the Creative Commons license, and indicate if changes were made. The images or other third party material in this article are included in the article’s Creative Commons license, unless indicated otherwise in a credit line to the material. If material is not included in the article’s Creative Commons license and your intended use is not permitted by statutory regulation or exceeds the permitted use, you will need to obtain permission directly from the copyright holder. To view a copy of this license, visit http://creativecommons.org/licenses/by/4.0/.
spellingShingle Article
Simões, Ana P.
Silva, Carla G.
Marques, Joana M.
Pochmann, Daniela
Porciúncula, Lisiane O.
Ferreira, Sofia
Oses, Jean P.
Beleza, Rui O.
Real, Joana I.
Köfalvi, Attila
Bahr, Ben A.
Lerma, Juan
Cunha, Rodrigo A.
Rodrigues, Ricardo J.
Glutamate-induced and NMDA receptor-mediated neurodegeneration entails P2Y1 receptor activation
title Glutamate-induced and NMDA receptor-mediated neurodegeneration entails P2Y1 receptor activation
title_full Glutamate-induced and NMDA receptor-mediated neurodegeneration entails P2Y1 receptor activation
title_fullStr Glutamate-induced and NMDA receptor-mediated neurodegeneration entails P2Y1 receptor activation
title_full_unstemmed Glutamate-induced and NMDA receptor-mediated neurodegeneration entails P2Y1 receptor activation
title_short Glutamate-induced and NMDA receptor-mediated neurodegeneration entails P2Y1 receptor activation
title_sort glutamate-induced and nmda receptor-mediated neurodegeneration entails p2y1 receptor activation
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5833818/
https://www.ncbi.nlm.nih.gov/pubmed/29463792
http://dx.doi.org/10.1038/s41419-018-0351-1
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