二甲双胍对近交系高饮酒黑暗品系1小鼠狂饮乙醇和单磷酸腺苷激酶信号转导的影响

IF 3 Q2 SUBSTANCE ABUSE
Kolter Grigsby, Jonathan Palacios, Amy E Chan, Sade M Spencer, Angela R Ozburn
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引用次数: 0

摘要

背景:单磷酸腺苷激活的蛋白激酶(AMPK)信号在调节全身细胞代谢和能量方面发挥着重要作用。乙醇和可卡因都会降低成瘾相关脑区的 AMPK 活性。虽然已发现激活 AMPK 可减少对可卡因的寻求,但其在有害饮酒和酒精使用障碍(AUD)进展中的作用仍不清楚。二甲双胍是一种靶向 AMPK 的 2 型糖尿病一线药物,我们想知道二甲双胍是否能减少近交系黑线高饮酒-1(iHDID-1)小鼠的狂饮型乙醇摄入量,黑线高饮酒-1 是一种饮酒致醉的遗传风险模型。然后,我们确定二甲双胍是否会改变 iHDID-1 小鼠的乙醇清除率。接下来,我们测试了二甲双胍和/或乙醇是否会改变脑核(NAc)中的AMPK信号转导,脑核是对有害饮酒至关重要的脑区:我们分别在急性(实验1)和慢性(实验3A)饮酒研究中测定了二甲双胍[0或250 mg/kg;腹腔注射(i.p.)]对暴饮型乙醇摄入的影响(n = 6-8 iHDID-1小鼠/性别/处理/实验)。在 iHDID-1 小鼠中测试了二甲双胍(0 或 250 毫克/千克)对乙醇(2.0 克/千克,静脉注射)清除率的影响(实验 2;n = 7-9/性别/处理)。最后,我们测量了NAc AMPK和磷酸化AMPK(pAMPK)水平对长期饮用乙醇(或水)(n = 6只iHDID-1小鼠/性别/治疗/流体类型;实验3B)和醉酒剂量乙醇(2.0 g/kg;i.p.;实验4)的反应:结果:在对雄性和雌性iHDID-1小鼠的急性和慢性研究中,二甲双胍都能减少狂饮乙醇的摄入量(P's):这些研究结果为二甲双胍这种经济、安全的糖尿病药物重新用于减少有害的乙醇摄入量提供了早期支持,并为测试其治疗 AUD 患者的疗效奠定了基础。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Effects of metformin on binge-like ethanol drinking and adenosine monophosphate kinase signaling in inbred high drinking in the dark line 1 mice.

Background: Adenosine monophosphate-activated protein kinase (AMPK) signaling plays a vital role in regulating cellular metabolism and energy throughout the body. Ethanol and cocaine both reduce AMPK activity in addiction-related brain regions. Though AMPK activation has been found to reduce cocaine seeking, its role in harmful drinking and alcohol use disorder (AUD) progression remains unclear. We asked whether metformin, a first-line type 2 diabetes medication that targets AMPK, can reduce binge-like ethanol intake in inbred High Drinking in the Dark Line-1 (iHDID-1) mice, a genetic risk model for drinking to intoxication. We then determined whether metformin altered ethanol clearance in iHDID-1 mice. Next, we tested whether metformin and/or ethanol altered AMPK signaling in the nucleus accumbens (NAc), a brain region critically important for harmful drinking.

Methods: We measured the effects of metformin [0 or 250 mg/kg; intraperitoneal injection (i.p.)] on binge-like ethanol intake in separate acute (Experiment 1) and chronic (Experiment 3A) drinking studies (n = 6-8 iHDID-1 mice/sex/treatment/experiment). The effect of metformin (0 or 250 mg/kg) on ethanol (2.0 g/kg, i.p.) clearance was tested in iHDID-1 mice (Experiment 2; n = 7-9/sex/treatment). Lastly, we measured NAc AMPK and phosphorylated AMPK (pAMPK) levels in response to chronic ethanol (or water) drinking (n = 6 iHDID-1 mice/sex/treatment/fluid type; Experiment 3B) and an intoxicating dose of ethanol (2.0 g/kg; i.p.; Experiment 4).

Results: Metformin reduced binge-like ethanol drinking intake in acute and chronic studies in both male and female iHDID-1 mice (p's < 0.05). We found no significant changes in ethanol clearance in response to metformin. Moreover, no differences in AMPK or pAMPK levels in the NAc were observed with either ethanol or metformin.

Conclusions: These findings provide early support for the repurposing of metformin, an affordable and safe diabetes medication, to reduce harmful ethanol intake and lay a foundation for testing its efficacy to treat individuals with AUD.

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