访问时间表调节高脂肪饮食对小鼠乙醇摄入和胰岛素及葡萄糖功能的影响。
Access schedules mediate the impact of high fat diet on ethanol intake and insulin and glucose function in mice.
机构信息
Department of Neural and Behavioral Science, Penn State College of Medicine, Hershey, PA, 17033, United States.
Department of Anesthesiology, Penn State College of Medicine, Hershey, PA, 17033, United States.
出版信息
Alcohol. 2020 Aug;86:45-56. doi: 10.1016/j.alcohol.2020.03.007. Epub 2020 Mar 26.
Alcoholism and high fat diet (HFD)-induced obesity individually promote insulin resistance and glucose intolerance in clinical populations, increasing risk for metabolic diseases. HFD can also stimulate alcohol intake in short-term clinical studies. Unfortunately, there is currently a disconnect between animal models and the clinical findings, as animal studies typically show that HFD decreases ethanol intake while ethanol intake mitigates HFD-induced effects on insulin and glucose dysfunction. However, most previous animal studies utilized forced or continuous HFD and/or ethanol. In three experiments we sought to determine whether HFD (HFD = 60% calories from fat) vs. control diet (chow = 16% fat) alters voluntary two-bottle choice ethanol intake in male C57Bl/6J mice given differing access schedules for 6-7 weeks, and we assessed the resultant impact on metabolic function via insulin and glucose tolerance tests. Experiment 1: Unlimited Access Ethanol + HFD (UAE + HFD; n = 15; 10% ethanol v/v, ad libitum diet and ethanol) or UAE + Chow (n = 15). Experiment 2: Limited Access Ethanol + HFD (LAE + HFD; n = 15; ethanol = 4 h/day; 3 days/week, ad libitum diet) or LAE + Chow (n = 15) with increasing ethanol concentrations (10%, 15%, 20%). Experiment 3: Intermittent HFD with limited access to ethanol (iHFD-E; HFD = single 24-h session/week; ethanol = 4 h/day; 4 days/week) (n = 10). UAE + HFD mice consumed significantly less ethanol and were insulin-resistant and hyperglycemic compared with UAE + Chow mice. LAE + HFD mice consumed ethanol similarly to LAE + Chow mice, but exhibited hyperglycemia, insulin resistance, and glucose intolerance. iHFD-E mice displayed binge eating-like behaviors and consumed significantly more ethanol than mice given ad libitum chow or HFD. iHFD-E mice did not have significantly altered body composition, but developed insulin insensitivity and glucose intolerance. These findings suggest that access schedules influence HFD effects on ethanol consumption and resultant metabolic dysfunction, ethanol intake does not improve HFD-induced metabolic dysfunction, and binge eating-like behaviors can transfer to binge drinking behaviors.
酒精中毒和高脂肪饮食(HFD)单独促进临床人群的胰岛素抵抗和葡萄糖耐量受损,增加代谢疾病的风险。HFD 还可以在短期临床研究中刺激酒精摄入。不幸的是,动物模型和临床发现之间存在脱节,因为动物研究通常表明 HFD 会降低乙醇摄入,而乙醇摄入减轻了 HFD 对胰岛素和葡萄糖功能障碍的影响。然而,大多数先前的动物研究使用强制或连续的 HFD 和/或乙醇。在三个实验中,我们试图确定 HFD(HFD=60%的热量来自脂肪)与对照饮食(chow=16%的脂肪)是否改变雄性 C57Bl/6J 小鼠在 6-7 周内给予不同摄入方案的自愿双瓶选择乙醇摄入,并通过胰岛素和葡萄糖耐量试验评估对代谢功能的影响。实验 1:无限量摄入酒精+HFD(UAE+HFD;n=15;10%乙醇 v/v,自由饮食和乙醇)或 UAE+Chow(n=15)。实验 2:有限量摄入酒精+HFD(LAE+HFD;n=15;乙醇=4 小时/天;每周 3 天,自由饮食)或 LAE+Chow(n=15),乙醇浓度增加(10%、15%、20%)。实验 3:间歇性 HFD 与有限量摄入乙醇(iHFD-E;HFD=每周 1 次 24 小时疗程;乙醇=4 小时/天;每周 4 天)(n=10)。与 UAE+Chow 小鼠相比,UAE+HFD 小鼠的乙醇摄入量明显减少,且胰岛素抵抗和高血糖。与 LAE+Chow 小鼠相比,LAE+HFD 小鼠的乙醇摄入量相似,但表现出高血糖、胰岛素抵抗和葡萄糖不耐受。iHFD-E 小鼠表现出暴饮暴食样行为,摄入的乙醇明显多于给予自由饮食或 HFD 的小鼠。iHFD-E 小鼠的身体成分没有明显改变,但出现胰岛素不敏感和葡萄糖不耐受。这些发现表明,摄入方案会影响 HFD 对乙醇摄入和由此产生的代谢功能障碍的影响,乙醇摄入不能改善 HFD 引起的代谢功能障碍,暴饮暴食样行为可以转移到狂饮行为。
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