1.Different development patterns of reward behaviors induced by ketamine and JWH-018 in striatal GAD67 knockdown mice
Sun Mi GU ; Eunchong HONG ; Sowoon SEO ; Sanghyeon KIM ; Seong Shoon YOON ; Hye Jin CHA ; Jaesuk YUN
Journal of Veterinary Science 2024;25(5):e63-
Objective:
The study was designed to examine the effects of the downregulation of GAD67 expression in the dorsal striatum on reward behavior development.
Methods:
We evaluated the effects of GAD67 knockdown on depression-like behavior and anxiety using the forced swim test and elevated plus maze test in a mouse model. We further determined the effects of GAD67 knockdown on ketamine- and JWH-018-induced conditioned place preference (CPP).
Results:
Knockdown of GAD67 in the dorsal striatum of mice increased depression-like behavior, but it decreased anxiety. Moreover, the CPP score on the NMDA receptor antagonist ketamine was increased by GAD67 knockdown, whereas the administration of JWH-018, a cannabinoid receptor agonist, did not affect the CPP score in the GAD67 knockdown mice group compared with the control group.
Conclusions
and Relevance: These results suggest that striatal GAD67 reduces GABAergic neuronal activity and may cause ketamine-induced NMDA receptor inhibition. Consequently, GAD67 downregulation induces vulnerability to the drug reward behavior of ketamine.
2.Different development patterns of reward behaviors induced by ketamine and JWH-018 in striatal GAD67 knockdown mice
Sun Mi GU ; Eunchong HONG ; Sowoon SEO ; Sanghyeon KIM ; Seong Shoon YOON ; Hye Jin CHA ; Jaesuk YUN
Journal of Veterinary Science 2024;25(5):e63-
Objective:
The study was designed to examine the effects of the downregulation of GAD67 expression in the dorsal striatum on reward behavior development.
Methods:
We evaluated the effects of GAD67 knockdown on depression-like behavior and anxiety using the forced swim test and elevated plus maze test in a mouse model. We further determined the effects of GAD67 knockdown on ketamine- and JWH-018-induced conditioned place preference (CPP).
Results:
Knockdown of GAD67 in the dorsal striatum of mice increased depression-like behavior, but it decreased anxiety. Moreover, the CPP score on the NMDA receptor antagonist ketamine was increased by GAD67 knockdown, whereas the administration of JWH-018, a cannabinoid receptor agonist, did not affect the CPP score in the GAD67 knockdown mice group compared with the control group.
Conclusions
and Relevance: These results suggest that striatal GAD67 reduces GABAergic neuronal activity and may cause ketamine-induced NMDA receptor inhibition. Consequently, GAD67 downregulation induces vulnerability to the drug reward behavior of ketamine.
3.Different development patterns of reward behaviors induced by ketamine and JWH-018 in striatal GAD67 knockdown mice
Sun Mi GU ; Eunchong HONG ; Sowoon SEO ; Sanghyeon KIM ; Seong Shoon YOON ; Hye Jin CHA ; Jaesuk YUN
Journal of Veterinary Science 2024;25(5):e63-
Objective:
The study was designed to examine the effects of the downregulation of GAD67 expression in the dorsal striatum on reward behavior development.
Methods:
We evaluated the effects of GAD67 knockdown on depression-like behavior and anxiety using the forced swim test and elevated plus maze test in a mouse model. We further determined the effects of GAD67 knockdown on ketamine- and JWH-018-induced conditioned place preference (CPP).
Results:
Knockdown of GAD67 in the dorsal striatum of mice increased depression-like behavior, but it decreased anxiety. Moreover, the CPP score on the NMDA receptor antagonist ketamine was increased by GAD67 knockdown, whereas the administration of JWH-018, a cannabinoid receptor agonist, did not affect the CPP score in the GAD67 knockdown mice group compared with the control group.
Conclusions
and Relevance: These results suggest that striatal GAD67 reduces GABAergic neuronal activity and may cause ketamine-induced NMDA receptor inhibition. Consequently, GAD67 downregulation induces vulnerability to the drug reward behavior of ketamine.
4.Different development patterns of reward behaviors induced by ketamine and JWH-018 in striatal GAD67 knockdown mice
Sun Mi GU ; Eunchong HONG ; Sowoon SEO ; Sanghyeon KIM ; Seong Shoon YOON ; Hye Jin CHA ; Jaesuk YUN
Journal of Veterinary Science 2024;25(5):e63-
Objective:
The study was designed to examine the effects of the downregulation of GAD67 expression in the dorsal striatum on reward behavior development.
Methods:
We evaluated the effects of GAD67 knockdown on depression-like behavior and anxiety using the forced swim test and elevated plus maze test in a mouse model. We further determined the effects of GAD67 knockdown on ketamine- and JWH-018-induced conditioned place preference (CPP).
Results:
Knockdown of GAD67 in the dorsal striatum of mice increased depression-like behavior, but it decreased anxiety. Moreover, the CPP score on the NMDA receptor antagonist ketamine was increased by GAD67 knockdown, whereas the administration of JWH-018, a cannabinoid receptor agonist, did not affect the CPP score in the GAD67 knockdown mice group compared with the control group.
Conclusions
and Relevance: These results suggest that striatal GAD67 reduces GABAergic neuronal activity and may cause ketamine-induced NMDA receptor inhibition. Consequently, GAD67 downregulation induces vulnerability to the drug reward behavior of ketamine.
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