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The role of hypothalamic peptide gene expression in alcohol self-administration behavior.

机译:下丘脑肽基因表达在酒精自我管理行为中的作用。

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Self-administration of ethanol and food share many common features and Richter hypothesized that an increase in ethanol consumption would decrease feeding to balance the excess calories contained in the ethanol. Previously, we have shown that individual alcohol consumption correlates with neurotransmitter gene expression, especially in the prefrontal cortex. To test the hypothesis of Richter, we measured hypothalamic gene expression of receptors or neuropeptides of known relevance for the regulation of food intake using qPCR and correlated this to individual ethanol consumption in Wistar rats. For validation, gene expression was first correlated with body weight. We found a correlation of dynorphin, somatostatin, melanocortin-4 receptor and serotonin 5-HT(2C) with body weight and trends to correlation for CART, thus confirming the established role of the hypothalamus in the regulation of weight. For ethanol consumption, correlations were found for CRH receptors 1 and 2 and vasopressin while strong trends were observed for galanin receptor 1, orexin receptor 1, MCH and adrenoceptor alpha(1B). Therefore, alcohol consumption does seem to involve several hypothalamic systems which also mediate feeding responses and suggests that the hypothalamus, together with the prefrontal cortex, may determine the 'stopping point' of an individual.
机译:乙醇和食物的自我管理具有许多共同特征,Richter认为,乙醇消耗量的增加会减少进食量,从而平衡乙醇中所含的过多卡路里。以前,我们已经表明,个体饮酒与神经递质基因表达有关,特别是在额叶前皮质。为了检验Richter的假设,我们使用qPCR测量了已知与食物摄入调控相关的受体或神经肽的下丘脑基因表达,并将其与Wistar大鼠的乙醇摄入量关联起来。为了验证,首先将基因表达与体重相关。我们发现强啡肽,生长抑素,黑皮质素4受体和5-羟色胺5-HT(2C)与体重和CART相关趋势相关,从而证实了下丘脑在体重调节中已确立的作用。对于乙醇的消耗,发现了CRH受体1和2与血管加压素的相关性,而甘丙肽受体1,食欲素受体1,MCH和肾上腺素受体α(1B)则观察到强烈的趋势。因此,饮酒似乎确实涉及几个下丘脑系统,这些系统也介导了进食反应,并表明下丘脑以及前额叶皮层可能决定了个体的“停止点”。

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