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Homer2 within the nucleus accumbens core bidirectionally regulates alcohol intake by both P and Wistar rats

机译:伏伏核核心内的Homer2双向调节P和Wistar大鼠的酒精摄入

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摘要

In murine models of alcoholism, the glutamate receptor scaffolding protein Homer2 bidirectionally regulates alcohol intake. Although chronic alcohol drinking increases Homer2 expression within the core subregion of the nucleus accumbens (NAc) of alcohol-preferring P rats, the relevance of this neuroadaptation for alcohol intake has yet to be determined in rats. Thus, the present study employed an adeno-associated viral vector (AAV) strategy to over-express and knock down the major rodent isoform Homer2b within the NAc of both P and outbred Wistar rats to examine for changes in alcohol preference and intake (0-30% v/v) under continuous-access procedures. The generalization of AAV effects to non-drug, palatable, sweet solutions was also determined in tests of sucrose (0-5% w/v) and saccharin (0-0.125% w/v) intake/preference. No net-flux in vivo microdialysis was conducted for glutamate in the NAc to relate Homer2-dependent changes in alcohol intake to extracellular levels of glutamate. Line differences were noted for sweet solution preference and intake, but these variables were not affected by intra-NAc AAV infusion in either line. In contrast, Homer2b over-expression elevated, while Homer2b knock-down reduced, alcohol intake in both lines, and this effect was greatest at the highest concentration. Strikingly, in P rats there was a direct association between changes in Homer2b expression and NAc extracellular glutamate levels, but this effect was not seen in Wistar rats. These data indicate that NAc Homer2b expression actively regulates alcohol consumption by rats, paralleling this previous observation in mice. Overall, these findings underscore the importance of mesocorticolimbic glutamate activity in alcohol abuse/dependence and suggest that Homer2b and/or its constituents may serve as molecular targets for the treatment of these disorders.
机译:在酒精中毒的小鼠模型中,谷氨酸受体支架蛋白Homer2双向调节酒精的摄入。虽然长期饮酒会增加嗜酒精的P大鼠伏隔核(NAc)核心子区域内Homer2的表达,但这种神经适应与酒精摄入的相关性尚待确定。因此,本研究采用了腺相关病毒载体(AAV)策略来过度表达和敲除P和近亲Wistar大鼠NAc中的主要啮齿动物同种型Homer2b,以检查酒精偏好和摄入量的变化(0- 30%v / v)。在蔗糖(0-5%w / v)和糖精(0-0.125%w / v)摄入/偏好试验中,还确定了AAV对非药物,可口的甜味溶液的影响的普遍性。在NAc中未对谷氨酸进行净通量体内微透析,以将酒精摄入的Homer2依赖性变化与细胞外谷氨酸水平相关联。注意到甜味溶液偏好和摄入量存在品系差异,但这些变量不受任一系中NAc AAV内输注的影响。相反,在两个系中,Homer2b的过表达均升高,而Homer2b的敲低降低,酒精摄入量增加,并且在最高浓度下这种作用最大。令人惊讶的是,在P大鼠中,Homer2b表达的变化与NAc细胞外谷氨酸水平之间存在直接关联,但在Wistar大鼠中未观察到这种作用。这些数据表明,NAc Homer2b的表达积极调节大鼠的饮酒量,与之前在小鼠中的观察结果相似。总体而言,这些发现强调了中皮质糖皮质激素谷氨酸活性在酒精滥用/依赖性中的重要性,并表明Homer2b和/或其成分可作为治疗这些疾病的分子靶标。

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