4.3 Article

The μ-opioid system in midline thalamic nuclei modulates defence strategies towards a conditioned fear stimulus in male mice

期刊

JOURNAL OF PSYCHOPHARMACOLOGY
卷 34, 期 11, 页码 1280-1288

出版社

SAGE PUBLICATIONS LTD
DOI: 10.1177/0269881120940919

关键词

Fear extinction; dorsal midline thalamus; mu-opioid receptor; opioids

资金

  1. Interdisciplinary Centre for Clinical Research (IZKF) [Jun3/003/17]
  2. German Research Foundation (Fear, Anxiety, Anxiety Disorders) [SFB-TRR 58 TP A08]

向作者/读者索取更多资源

Background: Nuclei located in the dorsal midline thalamus, such as the paraventricular nucleus of the thalamus (PVT), are crucial to modulate fear and aversive behaviour. In addition, the PVT shows a dense expression of mu-opioid receptors (MORs) and could mediate the anxiolytic effects of opioids. Methods: We analysed the contribution of MORs in the dorsal midline thalamus (i.e. the PVT) to the performance of mice in a classical fear conditioning paradigm. We locally injected a specific agonist (DAMGO), an antagonist (CTAP) of MOR or saline as a control into the dorsal midline thalamus of male mice, prior to fear extinction training. We assessed freezing as a typical measure of fear and extended our analysis by evaluation of aversive, non-aversive and neutral behavioural features using compositional data analysis. Results: Pharmacological blockade of MORs through CTAP in the dorsal midline thalamus induced a fear memory extinction deficit, as evidenced by maintained freezing during extinction sessions. Stimulation of MORs by DAMGO resulted in an overall increase in locomotor activity, associated with decreased freezing during recall of extinction. Compositional data analysis confirmed the freezing-related pharmacological effects and revealed specific differences in basic behavioural states. CTAP-treated mice remained in an aversive state, whereas DAMGO-treated mice displayed predominantly neutral behaviour. Conclusions: Fear extinction requires the integrity of the mu-opioid system in the dorsal midline thalamus. Pharmacological stimulation of MOR and associated facilitation of fear extinction recall suggest a potential therapeutic avenue for stress-related or anxiety disorders.

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