Edinger-Westphal Urocortin-1 Involvement in Binge Ethanol Intake and Reward

Edinger-Westphal Urocortin-1 参与暴饮暴食乙醇摄入和奖励

• 批准号: 8251695
• 负责人: William J Giardino
• 金额: $ 4.18万
• 依托单位: OREGON HEALTH & SCIENCE UNIVERSITY
• 依托单位国家: 美国
• 财政年份: 2011
• 资助国家: 美国
• 起止时间: 2011-12-01 至 2013-05-31
• 项目状态: 已结题
• 来源: https://reporter.nih.gov/project-details/8251695
• 关键词: Abstinence; Adult; Affect; Affinity; Alcohol abuse; Alcohol consumption; Alcohol dependence; Alcoholism; Alcohols; Animal Model; Area; Attenuated; Behavior; Behavioral; Behavioral Genetics; Behavioral Model; Binding; Blood; Brain; Brain region; Breeding; CARTPT gene; Cell Nucleus; Cocaine; Complex; Consumption; Corticotropin-Releasing Hormone; Corticotropin-Releasing Hormone Receptors; Cues; Development; Dopamine; Ethanol; FOS gene; Financial compensation; Gene Expression; Genes; Genetic Predisposition to Disease; Genetic Techniques; Heavy Drinking; Human; Individual; Infusion procedures; Intake; Knock-out; Knockout Mice; Laboratories; Lesion; Ligands; Light; Maps; Mediating; Methods; Modeling; Molecular Genetics; Mus; National Institute on Alcohol Abuse and Alcoholism; Neurons; Neuropeptides; Nucleus Accumbens; Operative Surgical Procedures; Oral; Outcome; Pattern; Phenotype; Play; Population; Predisposition; Procedures; Proteins; RNA Interference; Regulation; Relapse; Rewards; Rodent; Role; Self Administration; Site; Societies; Stress; Structure; Subfamily lentivirinae; System; Tactile; Technology; Testing; Tissues; Transcript; Ventral Tegmental Area; Viral; Virus; Wild Type Mouse; Work; alcohol reward; alcohol seeking behavior; alcohol use disorder; alcoholism therapy; base; binge drinking; brain pathway; conditioning; cost; drinking; endophenotype; ghrelin receptor; innovation; interest; knock-down; lentiviral-mediated; male; preference; problem drinker; receptor; relating to nervous system; research study; response; small hairpin RNA; tool; urocortin

Stress plays a key role in precipitating relapse to excessive ethanol (EtOH) consumption in dependent alcoholics. Even in non-dependent populations, evidence supports a role for neural stress networks, such as the corticotropin-releasing factor (CRF) system, in excessive EtOH intake. Unfortunately, the complex neuroanatomical and pharmacological features of the CRF system have hindered our understanding of the roles of its specific components in EtOH-related behaviors. To this end, we have devoted years of study to the examination of Urocortin-1 (Ucn1), an endogenous ligand of the CRF system that is closely related to the prototypical ligand CRF, yet binds to both CRF receptors with higher affinity than CRF itself. While the fields of alcohol abuse and addiction have typically focused on the mesolimbic dopamine pathway and brain structures such as the ventral tegmental area and nucleus accumbens, our laboratory has provided converging lines of evidence to support a role for the centrally-projecting neurons of the Edinger-Westphal nucleus (EWcp) in EtOH intake and sensitivity. The primary site of Ucn1 expression in the brain is within the EWcp, and a relationship between EWcp-Ucn1 expression and a genetic predisposition to excessive EtOH intake has been identified. Further interest in the EWcp as a brain region involved in EtOH intake is based on the observation that in addition to Ucn1, the cocaine- and amphetamine-regulated transcript (CART) neuropeptide, and the ghrelin receptor (Ghsr) are both highly expressed within EWcp. Intriguingly, these proteins have also been implicated in excessive EtOH consumption and EtOH-induced reward, and we have hypothesized that the role of the EWcp in excessive EtOH consumption is dependent on the interactions between Ucn1 and CART, Ghsr, and additional proteins. Thus, Specific Aim 1 of this proposal seeks to use quantitative PCR array technology elucidate interactions between Ucn1 and other EWcp-enriched genes that are relevant for EtOH-related behaviors, and Specific Aim 2 of my proposal seeks to examine well-characterized behavioral models of EtOH binge-drinking and EtOH- induced reward following knockdown of Ucn1 expression within the EWcp, using lentiviral-mediated RNA interference. These highly innovative experiments will not only conclusively determine the importance of EWcp-Ucn1 in two relevant behavioral endophenotypes of alcoholism, but will also use quantitative gene expression analyses to aid in unraveling the complex role that the EWcp plays in excessive EtOH intake.

压力在依赖性酗酒者过度酒精（EtOH）消费的复发中起关键作用。即使在非依赖性人群中，也有证据支持神经应激网络（如促肾上腺皮质激素释放因子（CRF）系统）在过量摄取EtOH中的作用。不幸的是，CRF系统复杂的神经解剖学和药理学特征阻碍了我们对其特定成分在etoh相关行为中的作用的理解。为此，我们花了多年的时间研究尿皮质素-1 (Ucn1)，这是一种CRF系统的内源性配体，与原型配体CRF密切相关，但与两种CRF受体结合的亲和力高于CRF本身。虽然酒精滥用和成瘾领域通常集中在中边缘多巴胺通路和大脑结构（如腹侧被盖区和伏核）上，但我们的实验室已经提供了越来越多的证据来支持Edinger-Westphal核（EWcp）的中央突出神经元在EtOH摄入和敏感性中的作用。大脑中Ucn1表达的主要位点在EWcp内，并且EWcp-Ucn1表达与过量摄取EtOH的遗传易感性之间的关系已被确定。对EWcp作为参与EtOH摄入的大脑区域的进一步研究是基于以下观察：除了Ucn1外，可卡因和安非他明调节的转录本（CART）神经肽和胃饥饿素受体（Ghsr）都在EWcp中高度表达。有趣的是，这些蛋白质也与过量的EtOH消耗和EtOH诱导的奖励有关，我们假设EWcp在过量的EtOH消耗中的作用取决于Ucn1与CART、Ghsr和其他蛋白质之间的相互作用。因此，本提案的Specific Aim 1旨在利用定量PCR阵列技术阐明Ucn1与其他与EtOH相关行为相关的富含EWcp的基因之间的相互作用，而我的提案的Specific Aim 2旨在利用慢病毒介导的RNA干扰，研究在EWcp内敲低Ucn1表达后，EtOH狂欢饮酒和EtOH诱导奖励的良好特征行为模型。这些极具创新性的实验不仅将最终确定EWcp- ucn1在酒精中毒的两种相关行为内表型中的重要性，而且还将使用定量基因表达分析来帮助揭示EWcp在过量摄取EtOH中所起的复杂作用。