表达μ阿片受体 A118G 多态性的“人源化”小鼠中乙醇饮用量增加是通过性别特异性机制介导的。
Increased ethanol drinking in "humanized" mice expressing the mu opioid receptor A118G polymorphism are mediated through sex-specific mechanisms.
机构信息
Department of Anesthesiology & Perioperative Medicine, Penn State University College of Medicine, Hershey, PA 17033, United States.
Department of Anesthesiology & Perioperative Medicine, Penn State University College of Medicine, Hershey, PA 17033, United States; Benedict College, Columbia, SC 29204, United States.
出版信息
Brain Res Bull. 2018 Apr;138:12-19. doi: 10.1016/j.brainresbull.2017.07.017. Epub 2017 Aug 2.
The A118G single nucleotide polymorphism (SNP) of the mu-opioid receptor gene (Oprm1) has been implicated in mediating the rewarding effects of alcohol. Clinical and preclinical studies suggest that the G allele may confer a genetic vulnerability to alcohol dependence, though it remains unknown whether these effects are sex-specific. We used male and female mice homozygous for the "humanized" 118AA or 118GG alleles to determine whether the A118G SNP potentiates ethanol consumption in a sex-specific manner in both the two-bottle choice and drinking-in-the-dark (DID) paradigms. Mice were also assessed for differences in naltrexone sensitivity, ethanol reward assessed via conditioned place preference (CPP), and sensitivity to the sedative/ataxic effects of ethanol using the rota-rod and loss of righting reflex (LORR) assays. We found that male and female 118GG mice drank significantly more ethanol than 118AA littermates using a continuous access, two-bottle choice paradigm. In the limited-access DID drinking model, (i) female (but not male) 118GG mice consumed more ethanol than 118AA mice and (ii) naltrexone pretreatment was equally efficacious at attenuating ethanol intake in both 118AA and 118GG female mice while having no effect in males. Male and female 118GG and female 118AA mice developed a robust conditioned place preference (CPP) for ethanol. Female 118GG mice displayed less sensitivity to the sedative/ataxic effects of ethanol compared to female 118AA mice on both the rota-rod and the LORR assays while male mice did not differ in their responses on either assay. Our findings suggest that increased ethanol consumption in male 118GG mice may be due to increased ethanol reward, while increased drinking in female 118GG mice might be due to decreased sensitivity to the sedative/ataxic effects of ethanol. Collectively, these data might be used to help identify sex-specific pharmacotherapies to combat alcohol use disorders.
阿 118G 单核苷酸多态性 (SNP) 的μ-阿片受体基因 (Oprm1) 已被牵连调解奖励作用的酒精。临床和临床前研究表明,G 等位基因可能赋予遗传易感性酒精依赖,尽管尚不清楚这些影响是否是性别特异性的。我们使用男性和女性小鼠纯合的"人性化"118AA 或 118GG 等位基因,以确定阿 118G SNP 是否增强乙醇消耗以性别特异性的方式在两个瓶选择和暗饮 (DID) 范式。还评估了小鼠在纳曲酮敏感性、乙醇奖励评估通过条件位置偏好 (CPP) 和敏感性镇静/共济失调的乙醇使用的转棒和失去翻正反射 (LORR) 试验。我们发现男性和女性 118GG 小鼠喝明显比 118AA 同窝小鼠更多的乙醇使用连续访问,两瓶选择范式。在有限访问 DID 饮酒模型,(一)女性 (但不是男性) 118GG 小鼠消耗更多的乙醇比 118AA 小鼠和 (ii) 纳曲酮预处理同样有效地减弱乙醇摄入量在 118AA 和 118GG 雌性小鼠而没有影响在男性。男性和女性 118GG 和女性 118AA 小鼠开发了一个强大的条件位置偏好 (CPP) 乙醇。女性 118GG 小鼠显示较少的敏感性镇静/共济失调的乙醇作用比女性 118AA 小鼠在转棒和 LORR 试验而男性小鼠在这两个试验没有不同的反应。我们的研究结果表明,增加乙醇消耗在男性 118GG 小鼠可能是由于增加乙醇奖励,而在女性 118GG 小鼠饮酒增加可能是由于减少敏感性镇静/共济失调的乙醇作用。总之,这些数据可以用来帮助识别性别特异性的药物治疗来对抗酒精使用障碍。
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