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糖皮质激素拮抗剂米非司酮对长期饮酒戒断后果的影响。

Effects of the glucocorticoid antagonist, mifepristone, on the consequences of withdrawal from long term alcohol consumption.

作者信息

Jacquot Catherine, Croft Adam P, Prendergast Mark A, Mulholland Patrick, Shaw Sidney G, Little Hilary J

机构信息

Department of Basic Medical Sciences, St George's, University of London, Cranmer Terrace, London, United Kingdom.

出版信息

Alcohol Clin Exp Res. 2008 Dec;32(12):2107-16. doi: 10.1111/j.1530-0277.2008.00799.x. Epub 2008 Sep 30.

Abstract

BACKGROUND

Studies were carried out to test the hypothesis that administration of a glucocorticoid Type II receptor antagonist, mifepristone (RU38486), just prior to withdrawal from chronic alcohol treatment, would prevent the consequences of the alcohol consumption and withdrawal in mice.

MATERIALS AND METHODS

The effects of administration of a single intraperitoneal dose of mifepristone were examined on alcohol withdrawal hyperexcitability. Memory deficits during the abstinence phase were measured using repeat exposure to the elevated plus maze, the object recognition test, and the odor habituation/discrimination test. Neurotoxicity in the hippocampus and prefrontal cortex was examined using NeuN staining.

RESULTS

Mifepristone reduced, though did not prevent, the behavioral hyperexcitability seen in TO strain mice during the acute phase of alcohol withdrawal (4 hours to 8 hours after cessation of alcohol consumption) following chronic alcohol treatment via liquid diet. There were no alterations in anxiety-related behavior in these mice at 1 week into withdrawal, as measured using the elevated plus maze. However, changes in behavior during a second exposure to the elevated plus maze 1 week later were significantly reduced by the administration of mifepristone prior to withdrawal, indicating a reduction in the memory deficits caused by the chronic alcohol treatment and withdrawal. The object recognition test and the odor habituation and discrimination test were then used to measure memory deficits in more detail, at between 1 and 2 weeks after alcohol withdrawal in C57/BL10 strain mice given alcohol chronically via the drinking fluid. A single dose of mifepristone given at the time of alcohol withdrawal significantly reduced the memory deficits in both tests. NeuN staining showed no evidence of neuronal loss in either prefrontal cortex or hippocampus after withdrawal from chronic alcohol treatment.

CONCLUSIONS

The results suggest mifepristone may be of value in the treatment of alcoholics to reduce their cognitive deficits.

摘要

背景

开展了多项研究以检验以下假设:在慢性酒精治疗停药前给予糖皮质激素II型受体拮抗剂米非司酮(RU38486),可预防小鼠酒精摄入及戒断的后果。

材料与方法

研究了腹腔注射单剂量米非司酮对酒精戒断性兴奋的影响。在禁欲期,通过重复暴露于高架十字迷宫、物体识别测试和气味习惯化/辨别测试来测量记忆缺陷。使用NeuN染色检查海马体和前额叶皮质的神经毒性。

结果

米非司酮减轻了(虽未预防)经液体饮食进行慢性酒精治疗后,TO品系小鼠在酒精戒断急性期(停止饮酒后4至8小时)出现的行为性兴奋。使用高架十字迷宫测量发现,这些小鼠在戒断1周时与焦虑相关的行为没有改变。然而,在停药前给予米非司酮可显著减少1周后再次暴露于高架十字迷宫时的行为变化,这表明慢性酒精治疗和戒断所导致的记忆缺陷有所减少。然后,在通过饮水长期给予酒精的C57/BL10品系小鼠酒精戒断后1至2周,使用物体识别测试以及气味习惯化和辨别测试更详细地测量记忆缺陷。在酒精戒断时给予单剂量米非司酮可显著减少两项测试中的记忆缺陷。NeuN染色显示,慢性酒精治疗停药后,前额叶皮质或海马体均无神经元丢失的迹象。

结论

结果表明,米非司酮可能对治疗酗酒者以减少其认知缺陷具有价值。

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