[摘要] Alcoholism is a chronic and progressive disorder characterized by periods of excessive drinking, withdrawal and abstinence, and eventual relapse. Both genetic and environmental factors contribute to the development of alcohol addiction, with stress being a critical environmental factor. Corticotropin-releasing hormone (CRH) is the key regulator of the mammalian stress response, and dysregulation of the CRH system is observed in binge drinking and alcohol dependence. CRH-binding protein (CRH-BP) is a secreted glycoprotein that binds CRH with a very high affinity, thereby regulating CRH receptor activation. Numerous studies have identified SNPs in the CRHBP gene that are associated with alcoholism, suggesting a role for CRH-BP in vulnerability to alcohol abuse.In this thesis, I investigated the role and regulation of CRH-BP in mouse models of binge drinking and alcohol dependence. Using in situ hybridization, I determined that repeated cycles of drinking in the dark, a mouse model of binge drinking, decrease CRH-BP mRNA expression in the medial prefrontal cortex, a region involved in executive function and regulation of emotion and behavior, including responses to stress. In a mouse model of alcohol dependence, the chronic intermittent ethanol (CIE) vapor paradigm, I observed a decrease in CRH-BP mRNA at peak alcohol withdrawal in the anterior paraventricular nucleus of the thalamus, a novel participant in the stress/reward circuitry. In a CIE paradigm that included periods of voluntary ethanol drinking, I detected a decrease in CRH-BP mRNA in the ventral tegmental area and an increase in CRH-BP mRNA in the bed nucleus of the stria terminalis, two key brain regions in the CRH and reward systems that have been implicated in control of excessive ethanol consumption. Interestingly, studies using CRH-BP KO mice suggest that the complete absence of CRH-BP may prevent increases in dependence-induced alcohol consumption.Together, these studies demonstrate changes in CRH-BP levels that may result in altered CRH receptor signaling within the stress and reward pathways in both binge drinking and dependence.I also examined the cell type-specific expression of CRH-BP in the PFC to begin to define the neural circuits in which CRH-BP is expressed. Using dual in situ hybridization, I detected CRH-BP mRNA predominantly in inhibitory, somatostatin-expressing interneurons of the PFC, suggesting that CRH-BP may be acting locally within the PFC to mediate its effects on CRH receptors on pyramidal neurons. These colocalization studies provide the basis for future studies to manipulate CRH-BP in a cell-type specific manner to further elucidate its role in mouse models of excessive alcohol consumption.Finally, I conducted signaling experiments that begin to address the mechanisms by which CRH-BP modulates CRH activity at the two CRH receptors. I demonstrated that CRH-BP inhibits CRH-mediated activation of CRH receptors and the resulting increases in cAMP in LβT2 cells, an effect that is partially reversed by the CRH-BP ligand inhibitor, CRH6-33. Lastly, I optimized a calcium assay for future experiments to assess CRH-BP modulation of CRH receptor signaling through the Gαq/PLC/PKC/calcium signaling pathway. Overall, the results from this thesis expand our knowledge on the role of the CRH-BP and the CRH system in alcohol use and addiction and begin to define the potential roles of CRH-BP within circuits of the stress and reward system and its mechanism of action.