有限度的过度自愿饮酒会导致小鼠肝功能障碍。
Limited Excessive Voluntary Alcohol Drinking Leads to Liver Dysfunction in Mice.
作者信息
Wegner Scott A, Pollard Katherine A, Kharazia Viktor, Darevsky David, Perez Luz, Roychowdhury Sanjoy, Xu Allison, Ron Dorit, Nagy Laura E, Hopf Frederic Woodward
机构信息
Department of Neurology, University of California at San Francisco, San Francisco, California.
Wheeler Center for the Study of Addiction, University of California at San Francisco, San Francisco, California.
出版信息
Alcohol Clin Exp Res. 2017 Feb;41(2):345-358. doi: 10.1111/acer.13303. Epub 2017 Jan 19.
BACKGROUND
Liver damage is a serious and sometimes fatal consequence of long-term alcohol intake, which progresses from early-stage fatty liver (steatosis) to later-stage steatohepatitis with inflammation and fibrosis/necrosis. However, very little is known about earlier stages of liver disruption that may occur in problem drinkers, those who drink excessively but are not dependent on alcohol.
METHODS
We examined how repeated binge-like alcohol drinking in C57BL/6 mice altered liver function, as compared with a single binge-intake session and with repeated moderate alcohol consumption. We measured a number of markers associated with early- and later-stage liver disruption, including liver steatosis, measures of liver cytochrome P4502E1 (CYP2E1) and alcohol dehydrogenase (ADH), alcohol metabolism, expression of cytokine mRNA, accumulation of 4-hydroxynonenal (4-HNE) as an indicator of oxidative stress, and alanine transaminase/aspartate transaminase as a measure of hepatocyte injury.
RESULTS
Importantly, repeated binge-like alcohol drinking increased triglyceride levels in the liver and plasma, and increased lipid droplets in the liver, indicators of steatosis. In contrast, a single binge-intake session or repeated moderate alcohol consumption did not alter triglyceride levels. In addition, alcohol exposure can increase rates of alcohol metabolism through CYP2E1 and ADH, which can potentially increase oxidative stress and liver dysfunction. Intermittent, excessive alcohol intake increased liver CYP2E1 mRNA, protein, and activity, as well as ADH mRNA and activity. Furthermore, repeated, binge-like drinking, but not a single binge or moderate drinking, increased alcohol metabolism. Finally, repeated, excessive intake transiently elevated mRNA for the proinflammatory cytokine IL-1B and 4-HNE levels, but did not alter markers of later-stage liver hepatocyte injury.
CONCLUSIONS
Together, we provide data suggesting that even relatively limited binge-like alcohol drinking can lead to disruptions in liver function, which might facilitate the transition to more severe forms of liver damage.
背景
肝损伤是长期饮酒的严重且有时致命的后果,其从早期脂肪肝(脂肪变性)发展为后期伴有炎症和纤维化/坏死的脂肪性肝炎。然而,对于问题饮酒者(即饮酒过量但不依赖酒精者)可能出现的肝脏破坏早期阶段,人们了解甚少。
方法
我们研究了与单次暴饮及反复适度饮酒相比,C57BL/6小鼠反复进行暴饮样饮酒如何改变肝功能。我们测量了一些与早期和后期肝脏破坏相关的指标,包括肝脏脂肪变性、肝细胞色素P4502E1(CYP2E1)和乙醇脱氢酶(ADH)的指标、酒精代谢、细胞因子mRNA表达、作为氧化应激指标的4-羟基壬烯醛(4-HNE)的积累以及作为肝细胞损伤指标的丙氨酸转氨酶/天冬氨酸转氨酶。
结果
重要的是,反复进行暴饮样饮酒会增加肝脏和血浆中的甘油三酯水平,并增加肝脏中的脂滴,这些都是脂肪变性的指标。相比之下,单次暴饮或反复适度饮酒不会改变甘油三酯水平。此外,酒精暴露可通过CYP2E1和ADH增加酒精代谢率,这可能会增加氧化应激和肝功能障碍。间歇性过量饮酒会增加肝脏CYP2E1的mRNA、蛋白质和活性,以及ADH的mRNA和活性。此外,反复进行暴饮样饮酒而非单次暴饮或适度饮酒会增加酒精代谢。最后,反复过量摄入会短暂升高促炎细胞因子IL-1B的mRNA和4-HNE水平,但不会改变后期肝脏肝细胞损伤的指标。
结论
总之,我们提供的数据表明,即使是相对有限的暴饮样饮酒也会导致肝功能紊乱,这可能会促进向更严重肝损伤形式的转变。
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