Up-Regulation of TREK-2 Potassium Channels in Cultured Astrocytes Requires De Novo Protein Synthesis: Relevance to Localization of TREK-2 Channels in Astrocytes after Transient Cerebral Ischemia

Excitotoxicity due to glutamate receptor over-activation is one of the key mediators of neuronal death after an ischemic insult. Therefore, a major function of astrocytes is to maintain low extracellular levels of glutamate. The ability of astrocytic glutamate transporters to regulate the extracellu...

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Autores principales: Rivera-Pagán, Aixa F., Rivera-Aponte, David E., Melnik-Martínez, Katya V., Zayas-Santiago, Astrid, Kucheryavykh, Lilia Y., Martins, Antonio H., Cubano, Luis A., Skatchkov, Serguei N., Eaton, Misty J.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2015
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Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4401746/
https://www.ncbi.nlm.nih.gov/pubmed/25886567
http://dx.doi.org/10.1371/journal.pone.0125195
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author Rivera-Pagán, Aixa F.
Rivera-Aponte, David E.
Melnik-Martínez, Katya V.
Zayas-Santiago, Astrid
Kucheryavykh, Lilia Y.
Martins, Antonio H.
Cubano, Luis A.
Skatchkov, Serguei N.
Eaton, Misty J.
author_facet Rivera-Pagán, Aixa F.
Rivera-Aponte, David E.
Melnik-Martínez, Katya V.
Zayas-Santiago, Astrid
Kucheryavykh, Lilia Y.
Martins, Antonio H.
Cubano, Luis A.
Skatchkov, Serguei N.
Eaton, Misty J.
author_sort Rivera-Pagán, Aixa F.
collection PubMed
description Excitotoxicity due to glutamate receptor over-activation is one of the key mediators of neuronal death after an ischemic insult. Therefore, a major function of astrocytes is to maintain low extracellular levels of glutamate. The ability of astrocytic glutamate transporters to regulate the extracellular glutamate concentration depends upon the hyperpolarized membrane potential of astrocytes conferred by the presence of K(+) channels in their membranes. We have previously shown that TREK-2 potassium channels in cultured astrocytes are up-regulated by ischemia and may support glutamate clearance by astrocytes during ischemia. Thus, herein we determine the mechanism leading to this up-regulation and assess the localization of TREK-2 channels in astrocytes after transient middle cerebral artery occlusion. By using a cell surface biotinylation assay we confirmed that functional TREK-2 protein is up-regulated in the astrocytic membrane after ischemic conditions. Using real time RT-PCR, we determined that the levels of TREK-2 mRNA were not increased in response to ischemic conditions. By using Western blot and a variety of protein synthesis inhibitors, we demonstrated that the increase of TREK-2 protein expression requires De novo protein synthesis, while protein degradation pathways do not contribute to TREK-2 up-regulation after ischemic conditions. Immunohistochemical studies revealed TREK-2 localization in astrocytes together with increased expression of the selective glial marker, glial fibrillary acidic protein, in brain 24 hours after transient middle cerebral occlusion. Our data indicate that functional TREK-2 channels are up-regulated in the astrocytic membrane during ischemia through a mechanism requiring De novo protein synthesis. This study provides important information about the mechanisms underlying TREK-2 regulation, which has profound implications in neurological diseases such as ischemia where astrocytes play an important role.
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spelling pubmed-44017462015-04-21 Up-Regulation of TREK-2 Potassium Channels in Cultured Astrocytes Requires De Novo Protein Synthesis: Relevance to Localization of TREK-2 Channels in Astrocytes after Transient Cerebral Ischemia Rivera-Pagán, Aixa F. Rivera-Aponte, David E. Melnik-Martínez, Katya V. Zayas-Santiago, Astrid Kucheryavykh, Lilia Y. Martins, Antonio H. Cubano, Luis A. Skatchkov, Serguei N. Eaton, Misty J. PLoS One Research Article Excitotoxicity due to glutamate receptor over-activation is one of the key mediators of neuronal death after an ischemic insult. Therefore, a major function of astrocytes is to maintain low extracellular levels of glutamate. The ability of astrocytic glutamate transporters to regulate the extracellular glutamate concentration depends upon the hyperpolarized membrane potential of astrocytes conferred by the presence of K(+) channels in their membranes. We have previously shown that TREK-2 potassium channels in cultured astrocytes are up-regulated by ischemia and may support glutamate clearance by astrocytes during ischemia. Thus, herein we determine the mechanism leading to this up-regulation and assess the localization of TREK-2 channels in astrocytes after transient middle cerebral artery occlusion. By using a cell surface biotinylation assay we confirmed that functional TREK-2 protein is up-regulated in the astrocytic membrane after ischemic conditions. Using real time RT-PCR, we determined that the levels of TREK-2 mRNA were not increased in response to ischemic conditions. By using Western blot and a variety of protein synthesis inhibitors, we demonstrated that the increase of TREK-2 protein expression requires De novo protein synthesis, while protein degradation pathways do not contribute to TREK-2 up-regulation after ischemic conditions. Immunohistochemical studies revealed TREK-2 localization in astrocytes together with increased expression of the selective glial marker, glial fibrillary acidic protein, in brain 24 hours after transient middle cerebral occlusion. Our data indicate that functional TREK-2 channels are up-regulated in the astrocytic membrane during ischemia through a mechanism requiring De novo protein synthesis. This study provides important information about the mechanisms underlying TREK-2 regulation, which has profound implications in neurological diseases such as ischemia where astrocytes play an important role. Public Library of Science 2015-04-17 /pmc/articles/PMC4401746/ /pubmed/25886567 http://dx.doi.org/10.1371/journal.pone.0125195 Text en © 2015 Rivera-Pagán et al http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Rivera-Pagán, Aixa F.
Rivera-Aponte, David E.
Melnik-Martínez, Katya V.
Zayas-Santiago, Astrid
Kucheryavykh, Lilia Y.
Martins, Antonio H.
Cubano, Luis A.
Skatchkov, Serguei N.
Eaton, Misty J.
Up-Regulation of TREK-2 Potassium Channels in Cultured Astrocytes Requires De Novo Protein Synthesis: Relevance to Localization of TREK-2 Channels in Astrocytes after Transient Cerebral Ischemia
title Up-Regulation of TREK-2 Potassium Channels in Cultured Astrocytes Requires De Novo Protein Synthesis: Relevance to Localization of TREK-2 Channels in Astrocytes after Transient Cerebral Ischemia
title_full Up-Regulation of TREK-2 Potassium Channels in Cultured Astrocytes Requires De Novo Protein Synthesis: Relevance to Localization of TREK-2 Channels in Astrocytes after Transient Cerebral Ischemia
title_fullStr Up-Regulation of TREK-2 Potassium Channels in Cultured Astrocytes Requires De Novo Protein Synthesis: Relevance to Localization of TREK-2 Channels in Astrocytes after Transient Cerebral Ischemia
title_full_unstemmed Up-Regulation of TREK-2 Potassium Channels in Cultured Astrocytes Requires De Novo Protein Synthesis: Relevance to Localization of TREK-2 Channels in Astrocytes after Transient Cerebral Ischemia
title_short Up-Regulation of TREK-2 Potassium Channels in Cultured Astrocytes Requires De Novo Protein Synthesis: Relevance to Localization of TREK-2 Channels in Astrocytes after Transient Cerebral Ischemia
title_sort up-regulation of trek-2 potassium channels in cultured astrocytes requires de novo protein synthesis: relevance to localization of trek-2 channels in astrocytes after transient cerebral ischemia
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4401746/
https://www.ncbi.nlm.nih.gov/pubmed/25886567
http://dx.doi.org/10.1371/journal.pone.0125195
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