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在大鼠中,血清微小RNA(miRNA)会因摄入乙醇和咖啡因而发生不同的变化。

Serum miRNAs are differentially altered by ethanol and caffeine consumption in rats.

作者信息

Martinez M, Rossetto I M U, Arantes R M S, Lizarte F S N, Tirapelli L F, Tirapelli D P C, Chuffa L G A, Martinez F E

机构信息

Department of Morphology and Pathology , Federal University of São Carlos (UFSCar) , São Carlos , SP , Brazil.

Department Structural and Functional Biology , University of Campinas (UNICAMP) , Campinas , SP , Brazil.

出版信息

Toxicol Res (Camb). 2019 Jul 17;8(6):842-849. doi: 10.1039/c9tx00069k. eCollection 2019 Nov 1.

Abstract

Alcoholism is a multifactorial disease with high risk for dependence determined by genetic background, environmental factors and neuroadaptations. The excessive consumption of this substance is related to psychiatric problems, epilepsy, cardiovascular disease, cirrhosis and cancers. Caffeine is one of the most popular psychostimulants currently consumed in the world. The combination of ethanol and caffeine ingested by consuming "energy drinks" is becoming increasingly popular among young people. We analyzed the effect of simultaneous consumption of ethanol and caffeine on the serum profile of differentially expressed in the ethanol-drinking rat model (UChB strain). Adult rats were divided into three groups ( = 5 per group): UChB group (rats fed with 1 : 10 (v/v) ethanol ); UChB + caffeine group (rats fed with 1 : 10 (v/v) ethanol + 3 g L of caffeine); control group (rats drinking water used as the control for UChB). The treatment with caffeine occurred from day 95 to 150 days old, totalizing 55 days of ethanol + caffeine ingestion. The expressions of microRNAs () -, -, -, -, - and - were detected by Real Time-PCR (RT-PCR). The expressions of , -, - and - were upregulated in the UChB group. Conversely, simultaneous ingestion of ethanol and caffeine significantly reversed these expressions to similar levels to control animals, thus emphasizing that caffeine had a protective effect in the presence of ethanol. In addition, was downregulated with ethanol consumption whereas miR- was unchanged. Ethanol and caffeine consumption was capable of altering serum miRNAs, which are potential biomarkers for the systemic effects of these addictive substances.

摘要

酒精中毒是一种多因素疾病,具有较高的依赖风险,其由遗传背景、环境因素和神经适应性决定。这种物质的过度消费与精神问题、癫痫、心血管疾病、肝硬化和癌症有关。咖啡因是目前世界上消费最广泛的精神兴奋剂之一。通过饮用“能量饮料”摄入乙醇和咖啡因的组合在年轻人中越来越受欢迎。我们分析了同时摄入乙醇和咖啡因对乙醇饮用大鼠模型(UChB品系)中差异表达的血清谱的影响。成年大鼠分为三组(每组 = 5只):UChB组(大鼠喂食1:10(v/v)乙醇);UChB + 咖啡因组(大鼠喂食1:10(v/v)乙醇 + 3 g/L咖啡因);对照组(大鼠饮用作为UChB对照的水)。咖啡因治疗从95日龄至150日龄进行,总共55天的乙醇 + 咖啡因摄入。通过实时定量聚合酶链反应(RT-PCR)检测微小RNA(miRNAs)-、-、-、-、-和-的表达。、-、-和-的表达在UChB组中上调。相反,同时摄入乙醇和咖啡因显著将这些表达逆转至与对照动物相似的水平,从而强调咖啡因在乙醇存在时有保护作用。此外,随着乙醇消费下调,而miR-不变。乙醇和咖啡因消费能够改变血清miRNAs,它们是这些成瘾物质全身效应的潜在生物标志物。

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