Inhibition of Potassium- and Ischemia-Evoked [3H] D-Aspartate Release from Isolated Bovine Retina by Cannabinoids

We investigated the effect of cannabinoids on potassium chloride (K+)- and ischemia-induced [3H]D-aspartate release from isolated bovine retinae. The superfusion method was employed for studies of [3H]-neurotransmitter release. Cannabinoid receptor CB1 agonists, but not the CB2 agonist JWH 015, inhi...

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Veröffentlicht in:	Current eye research 2006-01, Vol.31 (7-8), p.645-653
Hauptverfasser:	Opere, Catherine A., Zheng, Wei Dong, Zhao, Min, Lee, Jin Sook, Kulkarni, Kaustubh H., Ohia, Sunny E.
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Sprache:	eng
Schlagworte:	Animals aspartate Cannabinoids - pharmacology Cattle D-Aspartic Acid - antagonists & inhibitors D-Aspartic Acid - secretion Disease Models, Animal excitoxicity neuroprotection and inhibition In Vitro Techniques ischemia Ischemia - drug therapy Ischemia - metabolism Ischemia - pathology Potassium Chloride - pharmacology release Retina - drug effects Retina - metabolism Retina - pathology
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container_title	Current eye research
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creator	Opere, Catherine A. Zheng, Wei Dong Zhao, Min Lee, Jin Sook Kulkarni, Kaustubh H. Ohia, Sunny E.
description	We investigated the effect of cannabinoids on potassium chloride (K+)- and ischemia-induced [3H]D-aspartate release from isolated bovine retinae. The superfusion method was employed for studies of [3H]-neurotransmitter release. Cannabinoid receptor CB1 agonists, but not the CB2 agonist JWH 015, inhibited K+-induced [3H]D-aspartate release from bovine retinae with the following rank order of activity: anandamide > ACEA > methanandamide > WIN 55,212-2. In the ischemic model, the rank order of activity was as follows: methanandamide > ACEA > WIN 55,212-2. The CB1 receptor antagonist AM 251 blocked inhibitory responses produced by cannabinoids in both experimental conditions. In conclusion, cannabinoids inhibit evoked [3H]D-aspartate release from isolated bovine retinae via an effect on CB1 receptors.
doi_str_mv	10.1080/02713680600762747
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The superfusion method was employed for studies of [3H]-neurotransmitter release. Cannabinoid receptor CB1 agonists, but not the CB2 agonist JWH 015, inhibited K+-induced [3H]D-aspartate release from bovine retinae with the following rank order of activity: anandamide > ACEA > methanandamide > WIN 55,212-2. In the ischemic model, the rank order of activity was as follows: methanandamide > ACEA > WIN 55,212-2. The CB1 receptor antagonist AM 251 blocked inhibitory responses produced by cannabinoids in both experimental conditions. 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The superfusion method was employed for studies of [3H]-neurotransmitter release. Cannabinoid receptor CB1 agonists, but not the CB2 agonist JWH 015, inhibited K+-induced [3H]D-aspartate release from bovine retinae with the following rank order of activity: anandamide > ACEA > methanandamide > WIN 55,212-2. In the ischemic model, the rank order of activity was as follows: methanandamide > ACEA > WIN 55,212-2. The CB1 receptor antagonist AM 251 blocked inhibitory responses produced by cannabinoids in both experimental conditions. In conclusion, cannabinoids inhibit evoked [3H]D-aspartate release from isolated bovine retinae via an effect on CB1 receptors.</abstract><cop>England</cop><pub>Informa UK Ltd</pub><pmid>16877273</pmid><doi>10.1080/02713680600762747</doi><tpages>9</tpages></addata></record>
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subjects	Animals aspartate Cannabinoids - pharmacology Cattle D-Aspartic Acid - antagonists & inhibitors D-Aspartic Acid - secretion Disease Models, Animal excitoxicity neuroprotection and inhibition In Vitro Techniques ischemia Ischemia - drug therapy Ischemia - metabolism Ischemia - pathology Potassium Chloride - pharmacology release Retina - drug effects Retina - metabolism Retina - pathology
title	Inhibition of Potassium- and Ischemia-Evoked [3H] D-Aspartate Release from Isolated Bovine Retina by Cannabinoids
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