Hypoactive thalamic Crh+ cells in a female mouse model of alcohol drinking after social trauma
| Autor: | Kelly C. Burk, Klaus A. Miczek, Emily L. Newman, Michael Z. Leonard, Herbert E. Covington |
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| Jazyk: | angličtina |
| Rok vydání: | 2021 |
| Předmět: |
Alcohol Drinking
Corticotropin-Releasing Hormone media_common.quotation_subject Population Thalamus Binge drinking Receptors Corticotropin-Releasing Hormone Article Mice Corticotropin-releasing hormone Animals Medicine Humans education Biological Psychiatry media_common Neurons education.field_of_study Ethanol business.industry Cognition Abstinence Social relation Alcoholism Mood Female business Neuroscience Stress Psychological |
| Zdroj: | Biol Psychiatry |
| Popis: | Background Comorbid stress-induced mood and alcohol use disorders are increasingly prevalent among female patients. Stress exposure can disrupt salience processing and goal-directed decision making, contributing to persistent maladaptive behavioral patterns; these and other stress-sensitive cognitive and behavioral processes rely on dynamic and coordinated signaling by midline and intralaminar thalamic nuclei. Considering the role of social trauma in the trajectory of these debilitating psychopathologies, identifying vulnerable thalamic cells may provide guidance for targeting persistent stress-induced symptoms. Methods A novel behavioral protocol traced the progression from social trauma to the development of social defensiveness and chronically escalated alcohol consumption in female mice. Recent cell activation—measured as cFos—was quantified in thalamic cells after safe social interactions, revealing stress-sensitive corticotropin-releasing hormone–expressing (Crh+) anterior central medial thalamic (aCMT) cells. These cells were optogenetically stimulated during stress-induced social defensiveness and abstinence-escalated binge drinking. Results Crh+ aCMT neurons exhibited substantial activation after social interactions in stress-naive but not in stressed female mice. Photoactivating Crh+ aCMT cells dampened stress-induced social deficits, whereas inhibiting these cells increased social defensiveness in stress-naive mice. Optogenetically activating Crh+ aCMT cells diminished abstinence-escalated binge alcohol drinking in female mice, regardless of stress history. Conclusions This work uncovers a role for Crh+ aCMT neurons in maladaptive stress-induced social interactions and in binge drinking after forced abstinence in female mice. This molecularly defined thalamic cell population may serve as a critical stress-sensitive hub for social deficits caused by exposure to social trauma and for patterns of excessive alcohol drinking in female populations. |
| Databáze: | OpenAIRE |
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