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急性 binge 饮酒会改变整个身体的代谢,并且在小鼠体内持续多日改变骨骼肌特异性代谢标志物的时间依赖性表达。

Acute binge alcohol alters whole body metabolism and the time-dependent expression of skeletal muscle-specific metabolic markers for multiple days in mice.

机构信息

Department of Nutrition and Integrative Physiology, Florida State University, Tallahassee, Florida.

Department of Biological Science, Program in Neuroscience, and Institute of Molecular Biophysics, Florida State University, Tallahassee, Florida.

出版信息

Am J Physiol Endocrinol Metab. 2022 Sep 1;323(3):E215-E230. doi: 10.1152/ajpendo.00026.2022. Epub 2022 Jul 6.

Abstract

Alcohol is a myotoxin that disrupts skeletal muscle function and metabolism, but specific metabolic alternations following a binge and the time course of recovery remain undefined. The purpose of this work was to determine the metabolic response to binge alcohol, the role of corticosterone in this response, and whether nutrient availability mediates the response. Female mice received saline (control) or alcohol (EtOH) (5 g/kg) via intraperitoneal injection at the start of the dark cycle. Whole body metabolism was assessed for 5 days. In a separate cohort, gastrocnemius muscles and liver were collected every 4 h for 48 h following intoxication. Metyrapone was administered before alcohol and gastrocnemius was collected 4 h later. Lastly, alcohol-treated mice were compared with fed or fasted controls. Alcohol disrupted whole body metabolism for multiple days. Alcohol altered the expression of genes and proteins in the gastrocnemius related to the promotion of fat oxidation (, AMPK, and ) and protein breakdown (, ). Changes to select metabolic genes in the liver did not parallel those in skeletal muscle. An alcohol-induced increase in circulating corticosterone was responsible for the initial change in protein breakdown factors but not the induction of , and . Alcohol led to a similar, but distinct metabolic response when compared with fasting animals. Overall, these data show that an acute alcohol binge rapidly disrupts macronutrient metabolism including sustained disruption to the metabolic gene signature of skeletal muscle in a manner similar to fasting at some time points. Herein, we demonstrate that acute alcohol intoxication immediately alters whole body metabolism coinciding with rapid changes in the skeletal muscle macronutrient gene signature for at least 48 h postbinge and that this response diverges from hepatic effects and those of a fasted animal.

摘要

酒精是一种肌肉毒素,会破坏骨骼肌功能和代谢,但 binge 后特定的代谢改变和恢复时间仍不清楚。本研究的目的是确定 binge 酒精后的代谢反应、皮质酮在此反应中的作用,以及营养供应是否调节该反应。雌性小鼠在暗周期开始时通过腹腔注射接受生理盐水(对照)或酒精(EtOH)(5 g/kg)。在接下来的 5 天中评估全身代谢。在另一组中,在中毒后 48 小时内每隔 4 小时收集腓肠肌和肝脏。在酒精前给予 metyrapone,并在 4 小时后收集腓肠肌。最后,将酒精处理的小鼠与进食或禁食对照进行比较。酒精会使全身代谢在多日发生紊乱。酒精改变了腓肠肌中与促进脂肪氧化(、AMPK 和)和蛋白质分解(、)相关的基因和蛋白质的表达。肝脏中某些代谢基因的变化与骨骼肌的变化不同步。酒精诱导的循环皮质酮增加是导致最初蛋白质分解因子变化的原因,但不是诱导、和的原因。与禁食动物相比,酒精引起的代谢反应相似但不同。总体而言,这些数据表明,急性酒精 binge 会迅速破坏 Macronutrient 代谢,包括在某些时间点以类似于禁食的方式持续破坏骨骼肌的代谢基因特征。在这里,我们证明急性酒精中毒会立即改变全身代谢,同时腓肠肌 Macronutrient 基因特征迅速发生变化,至少在 binge 后 48 小时内如此,并且该反应与肝效应和禁食动物的反应不同。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/25be/9423784/9a143a41ba73/e-00026-2022r01.jpg

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