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首页> 外文期刊>Toxicology in vitro: an international journal published in association with BIBRA >Effect of chronic ethanol exposure on the hepatotoxicity of ecstasy in mice: an ex vivo study.
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Effect of chronic ethanol exposure on the hepatotoxicity of ecstasy in mice: an ex vivo study.

机译:长期乙醇暴露对小鼠摇头丸肝毒性的影响:一项离体研究。

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摘要

3,4-Methylenedioxymethamphetamine (MDMA) is frequently consumed at "rave" parties by polydrug users that usually take this drug in association with ethanol. In addition, many young people are repeatedly exposed to ethanol, which likely leads to tolerance phenomena. Both compounds are metabolized in the liver, with formation of hepatotoxic metabolites, which gives high relevance to the evaluation of their putative toxicological interaction. Therefore, the aim of this study was to evaluate the toxicity induced by 0.8 and 1.6 mM MDMA to freshly isolated hepatocytes obtained from ethanol-treated mice whose tap drinking water was replaced by a 5% ethanol solution for 1 week and, afterwards, by a 12% ethanol solution for 8 weeks (ethanol group) comparatively to non-treated animals (non-ethanol group). The hepatocytes were incubated under normothermic and hyperthermic conditions in order to simulate in vitro the hyperthermic response induced in vivo by MDMA, a condition that has been recognized as a life-threatening effect associated with MDMA exposure and implicated in its hepatotoxicity. Six mice treated under the same protocol as the ethanol group were used for histological analysis, and compared to non-ethanol-treated animals. The pre-treatment of mice with ethanol caused a significant decrease in the hepatocytes yield in the isolation procedure comparatively to the non-ethanol group, which can be explained by an increase in collagen deposition along the hepatic parenchyma as observed in the histological analysis. The initial cell viability of hepatocytes suspensions was similar between ethanol and non-ethanol groups. However, the ethanol group showed a higher GSH oxidation rate, which was enhanced under hyperthermia. Additionally, a concentration-dependent MDMA-induced loss of cell viability and ATP depletion was observed for both groups, at 41 degrees C. In conclusion, the repeated treatment with ethanol seems to increase the vulnerability of freshly isolated mice hepatocytes towards pro-oxidant conditions, as ascertained by the increase in collagen deposition, lower hepatocyte yield and decreased glutathione levels. However, MDMA toxicity to the isolated hepatocytes was independent of ethanol pre-treatment, while significantly dependent on incubation temperature.
机译:3,4-亚甲二氧基甲基苯丙胺(MDMA)通常在“狂欢”聚会上被多药使用者服用,他们通常将这种药物与乙醇一起服用。另外,许多年轻人反复暴露于乙醇中,这很可能导致耐受现象。两种化合物均在肝脏中代谢,形成肝毒性代谢产物,这与评估其假定的毒理学相互作用具有高度相关性。因此,本研究的目的是评估0.8和1.6 mM MDMA对新鲜分离的肝细胞的毒性,该肝细胞得自于用5%乙醇溶液代替自来水的乙醇处理小鼠1周,然后再用与未经处理的动物(非乙醇组)相比,在12%的乙醇溶液中放置8周(乙醇组)。在常温和高温条件下孵育肝细胞,以在体外模拟由MDMA体内诱导的高温响应,MDMA是一种公认​​的与MDMA暴露相关的威胁生命的作用,并涉及其肝毒性。用与乙醇组相同的方案处理的六只小鼠用于组织学分析,并与未乙醇处理的动物进行比较。与非乙醇组相比,用乙醇预处理的小鼠在分离过程中引起肝细胞产率的显着降低,这可以通过组织学分析中观察到的沿肝实质的胶原沉积增加来解释。肝细胞悬液的初始细胞活力在乙醇和非乙醇组之间相似。但是,乙醇基团显示较高的GSH氧化速率,在高温下可提高该氧化速率。此外,在41摄氏度时,两组均观察到了浓度依赖性的MDMA诱导的细胞活力丧失和ATP消耗。总而言之,用乙醇反复处理似乎增加了新鲜分离的小鼠肝细胞对促氧化剂条件的脆弱性。由胶原蛋白沉积增加,肝细胞产量降低和谷胱甘肽水平降低确定。但是,MDMA对分离的肝细胞的毒性与乙醇预处理无关,而在很大程度上取决于孵育温度。

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