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反复给予地西泮可逆转短期而非长期戒酒期后前额叶皮质的工作记忆损伤和糖皮质激素改变。

Repeated diazepam administration reversed working memory impairments and glucocorticoid alterations in the prefrontal cortex after short but not long alcohol-withdrawal periods.

作者信息

Dominguez G, Henkous N, Pierard C, Belzung C, Mons N, Beracochea Daniel

机构信息

Université de Bordeaux, INCIA CNRS UMR 5287, Bat B2, Allée Geoffroy St Hilaire, CS 50023, 33615, Pessac, France.

Université François Rabelais, Inserm U930, Parc Grandmont, 37200, Tours, France.

出版信息

Cogn Affect Behav Neurosci. 2018 Aug;18(4):665-679. doi: 10.3758/s13415-018-0595-3.

Abstract

The study was designed to assess whether repeated administration of diazepam (Valium®, Roche)-a benzodiazepine exerting an agonist action on GABA receptors-may alleviate both the short (1 week, 1W) and long-term (6 weeks, 6W) deleterious effects of alcohol withdrawal occurring after chronic alcohol consumption (6 months; 12% v/v) in C57/BL6 male mice. More pointedly, we first evidenced that 1W and 6W alcohol-withdrawn mice exhibited working memory deficits in a sequential alternation task, associated with sustained exaggerated corticosterone rise and decreased pCREB levels in the prefrontal cortex (PFC). In a subsequent experiment, diazepam was administered i.p. for 9 consecutive days (1 injection/day) during the alcohol withdrawal period at decreasing doses ranging from 1.0 mg/kg to 0.25 mg/kg. Diazepam was not detected in the blood of withdrawn mice at the time of memory testing, occurring 24 hours after the last diazepam injection. Repeated diazepam administration significantly improved alternation rates and normalized levels of glucocorticoids and pCREB activity in the PFC in 1W but not in 6W withdrawn mice. Thus, repeated diazepam administration during the alcohol-withdrawal period only transitorily canceled out the working memory impairments and glucocorticoid alterations in the PFC of alcohol-withdrawn animals.

摘要

本研究旨在评估反复给予地西泮(安定,罗氏公司生产)——一种对GABA受体起激动作用的苯二氮䓬类药物——是否能减轻C57/BL6雄性小鼠长期(6个月;12% v/v)摄入酒精后出现的短期(1周,1W)和长期(6周,6W)酒精戒断的有害影响。更确切地说,我们首先证明,1W和6W酒精戒断小鼠在连续交替任务中表现出工作记忆缺陷,这与前额叶皮质(PFC)中持续过度的皮质酮升高和pCREB水平降低有关。在随后的实验中,在酒精戒断期间,以1.0 mg/kg至0.25 mg/kg的递减剂量腹腔注射地西泮,连续9天(每天1次注射)。在最后一次注射地西泮24小时后进行记忆测试时,在戒断小鼠的血液中未检测到地西泮。反复给予地西泮可显著提高1W酒精戒断小鼠的交替率,并使PFC中的糖皮质激素水平和pCREB活性恢复正常,但对6W酒精戒断小鼠无效。因此,在酒精戒断期间反复给予地西泮只能暂时消除酒精戒断动物PFC中的工作记忆损害和糖皮质激素改变。

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