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首页> 外文期刊>Psychopharmacology >The effects of repeated zolpidem treatment on tolerance, withdrawal-like symptoms, and GABAA receptor mRNAs profile expression in mice: Comparison with diazepam
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The effects of repeated zolpidem treatment on tolerance, withdrawal-like symptoms, and GABAA receptor mRNAs profile expression in mice: Comparison with diazepam

机译:重复唑吡坦治疗对小鼠耐受性,戒断样症状和GABAA受体mRNA表达的影响:与地西epa比较

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摘要

Rationale: Zolpidem is a short-acting, non-benzodiazepine hypnotic that acts as a full agonist at α1-containing GABAA receptors. Overall, zolpidem purportedly has fewer instances of abuse and dependence than traditionally used benzodiazepines. However, several studies have shown that zolpidem may be more similar to benzodiazepines in terms of behavioral tolerance and withdrawal symptoms. Objectives: In the current study, we examined whether subchronic zolpidem or diazepam administration produced deficits in zolpidem's locomotor-impairing effects, anxiety-like behaviors, and changes in GABA AR subunit messenger RNA (mRNA). Methods: Mice were given subchronic injections of either zolpidem (10 mg/kg), diazepam (20 mg/kg), or vehicle twice daily for 7 days. On day 8, mice were given a challenge dose of zolpidem (2 mg/kg) or vehicle before open field testing. Another set of mice underwent the same injection regimen but were sacrificed on day 8 for qRT-PCR analysis. Results: We found that subchronic zolpidem and diazepam administration produced deficits in the acute locomotor-impairing effects of zolpidem and increased anxiety-like behaviors 1 day after drug termination. In addition, we found that subchronic treatment of zolpidem and diazepam induced distinct but overlapping GABAAR subunit mRNA changes in the cortex but few changes in the hippocampus, amygdala, or prefrontal cortex. Levels of mRNA measured in separate mice after a single injection of either zolpidem or diazepam revealed no mRNA changes. Conclusions: In mice, subchronic treatment of zolpidem and diazepam can produce deficits in the locomotor-impairing effects of zolpidem, anxiety-like withdrawal symptoms, and subunit-specific mRNA changes.
机译:原理:唑吡坦是一种短效的非苯二氮杂类催眠药,对含α1的GABAA受体具有完全的激动作用。总体而言,据称唑吡坦比传统使用的苯二氮卓类具有更少的滥用和依赖性实例。但是,一些研究表明,唑吡坦在行为耐受性和戒断症状方面可能与苯二氮卓类药物更为相似。目的:在当前研究中,我们检查了亚慢性唑吡坦或地西epa的给药是否会导致唑吡坦的运动障碍作用,焦虑样行为以及GABA AR亚基信使RNA(mRNA)的变化缺乏。方法:每天两次给小鼠亚唑吡坦(10mg / kg),地西epa(20mg / kg)或赋形剂亚慢性注射,共7天。在第8天,在野外测试之前,给小鼠挑战剂量的唑吡坦(2 mg / kg)或赋形剂。另一组小鼠接受相同的注射方案,但是在第8天处死用于qRT-PCR分析。结果:我们发现亚慢性唑吡坦和地西epa的给药在药物终止后1天导致唑吡坦的急性运动损害作用出现不足,并增加了类似焦虑的行为。此外,我们发现亚唑吡坦和地西epa的亚慢性治疗在皮质中引起明显但重叠的GABAAR亚基mRNA变化,但在海马,杏仁核或前额叶皮质中变化很小。单次注射唑吡坦或地西epa后,在单独的小鼠中测得的mRNA水平未发现mRNA的变化。结论:在小鼠中,亚唑吡坦和地西epa的亚慢性治疗可导致唑吡坦的运动损伤作用,焦虑样戒断症状和亚基特异性mRNA变化不足。

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