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• W2022279968 endingPage "2033" @default.
• W2022279968 startingPage "2024" @default.
• W2022279968 abstract "Activation of cannabinoid CB1 receptor is shown to inhibit marble-burying behavior (MBB), a behavioral model for assessing obsessive-compulsive disorder (OCD). Anandamide, an endogenous agonist at CB1 receptor also activates the transient receptor potential vanilloid type 1 (TRPV1) channels but at a higher concentration. Furthermore, anandamide-mediated TRPV1 effects are opposite to that of the CB1 receptor. Therefore, the present study was carried out to investigate the influence of low and high doses of anandamide on MBB in CB1 and TRPV1 antagonist pre-treated mice. The results revealed that i.c.v. administration of lower doses of anandamide (1–10 μg/mouse) or its analogues (AM404 or URB597; 1–5 μg/mouse) inhibited MBB indicating the anticompulsive activity. Conversely, at higher doses (40 or 20 μg/mouse) these compounds increased MBB similar to capsaicin (TRPV1 agonist, 100 μg/mouse) exhibiting a pro-compulsive effect. Pretreatment with AM251 (CB1 antagonist, 1 μg/mouse) antagonized the anticompulsive effect of these compounds, while their pro-compulsive effect at higher doses was attenuated by inactive dose of capsazepine (TRPV1 antagonist, 10 μg/mouse). However, capsazepine per se at a higher dose (100 μg/mouse) inhibited MBB. When given daily for 14 days, the anticompulsive effect of anandamide and its analogues gradually disappeared, whereas capsazepine either alone or with URB597 produced consistent inhibition of MBB comparable to fluoxetine. Thus, the study indicates the biphasic influence of anandamide on MBB, and chronic administration of capsazepine either alone or with URB597 might be an effective tool in the treatment of OCD." @default.
• W2022279968 created "2016-06-24" @default.
• W2022279968 creator A5023973459 @default.
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• W2022279968 date "2012-04-01" @default.
• W2022279968 modified "2023-09-23" @default.
• W2022279968 title "Endocannabinoid analogues exacerbate marble-burying behavior in mice via TRPV1 receptor" @default.
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• W2022279968 doi "https://doi.org/10.1016/j.neuropharm.2011.12.030" @default.
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