Sex-Specific Regulation of Depression, Anxiety-Like Behaviors and Alcohol Drinking in Mice Lacking ENT1.

Christina L Ruby, Denise L Walker, Joyce An, Jason Kim, Doo-Sup Choi
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引用次数: 11

Abstract

OBJECTIVES: Adenosine signaling has been implicated in the pathophysiology of several psychiatric disorders including alcoholism, depression, and anxiety. Adenosine levels are controlled in part by transport across the cell membrane by equilibrative nucleoside transporters (ENTs). Recent evidence showed that a polymorphism in the gene encoding ENT1 is associated with comorbid depression and alcoholism in women. We have previously shown that deletion of ENT1 reduces ethanol intoxication and elevates alcohol intake in mice. Interestingly, ENT1 null mice display decreased anxiety-like behavior compared to wild-type littermates. However, our behavioral studies were performed only in male mice. Here, we extend our research to include female mice, and test the effect of ENT1 knockout on other behavioral correlates of alcohol drinking, including depressive and compulsive behavior, in mice. METHODS: To assess depression-like behavior, we used a forced swim test modified for mice. We examined anxiety-like behavior and locomotor activity in open field chambers, and perseverant behavior using the marble-burying test. Finally, we investigated alcohol consumption and preference in female mice using a two-bottle choice paradigm. RESULTS: ENT1 null mice of both sexes showed reduced immobility time in the forced swim test and increased time in the center of the open field compared to wild-type littermates. ENT1 null mice of both sexes showed similar locomotor activity levels and habituation to the open field chambers. Female ENT1 null mice displayed increased marble-burying compared to female wild-types, but no genotype difference was evident in males. Female ENT1 null mice showed increased ethanol consumption and preference compared to female wild-types. CONCLUSIONS: Our findings suggest that ENT1 contributes to several important behaviors involved in psychiatric disorders. Inhibition of ENT1 may be beneficial in treating depression and anxiety, while enhancement of ENT1 function may reduce compulsive behavior and drinking, particularly in females.

缺乏ENT1小鼠抑郁、焦虑样行为和饮酒的性别特异性调节
目的:腺苷信号传导与包括酒精中毒、抑郁和焦虑在内的几种精神疾病的病理生理有关。腺苷水平在一定程度上受平衡核苷转运体(ENTs)在细胞膜上的转运控制。最近的证据表明,编码ENT1基因的多态性与女性抑郁症和酒精中毒的共病有关。我们之前已经证明,在小鼠中,删除ENT1可以减少乙醇中毒并增加酒精摄入量。有趣的是,与野生型幼崽相比,ENT1缺失小鼠表现出的焦虑样行为有所减少。然而,我们的行为研究仅在雄性小鼠中进行。在这里,我们将我们的研究扩展到雌性小鼠,并测试ENT1敲除对饮酒的其他行为相关的影响,包括小鼠的抑郁和强迫行为。方法:为了评估抑郁样行为,我们使用了改良的小鼠强迫游泳测试。我们用埋弹试验检测了开放性实验室内的焦虑样行为和运动活动,以及持之以恒的行为。最后,我们使用两瓶选择范式研究了雌性小鼠的酒精消耗和偏好。结果:与野生型仔鼠相比,ENT1阴性小鼠在强迫游泳测试中静止时间减少,在开放场地中心的时间增加。两种性别的ENT1无效小鼠表现出相似的运动活动水平和对开放野室的习惯。与雌性野生型相比,雌性ENT1缺失小鼠显示出更多的大理石掩埋,但在雄性中没有明显的基因型差异。与雌性野生型相比,雌性ENT1缺失小鼠表现出更高的乙醇消耗和偏好。结论:我们的研究结果表明,ENT1参与了精神疾病的几个重要行为。抑制ENT1可能对治疗抑郁和焦虑有益,而增强ENT1功能可能减少强迫行为和饮酒,特别是在女性中。
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