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Zolpidem withdrawal delirium, seizure, and acute psychosis: Case reports and literature review

机译:Zolpidem退出谵妄,癫痫发作和急性精神病:案例报告和文献综述

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摘要

Zolpidem, a non-benzodiazepine hypnotic drug, shows a high affinity for the BZ1 (wl) subtypes of the modulatory sites within the GABAA receptor complex, but classical benzodiazepines (diazepam, lorazepam) have a non-specific affinity profile at wl and w>2 subtypes of the GABAA receptor. Therefore, zolpidem is thought to be safer than benzodiazepines. We present five cases with withdrawal delirium, seizure, acute psychosis and orofacial dyskinesia that developed following cessation of zolpidem. Adverse effects such as withdrawal seizure and withdrawal delirium have been rarely reported in relation to zolpidem. Chemically unrelated to benzodiazepines, zolpidem is thought to have fewer adverse effects, but shares a pharmacokinetic profile with the benzodiazepines. It is advised that the normal criteria for the prescription of benzodiazepines also be used when prescribing non-benzodiazepine sedatives and hypnotics, as they act upon the same receptor, namely, the benzo-diazepine-GABA-chloride complex. However, at higher than recommended doses for extended periods of time, the addictive potential of zolpidem may be similar to that of the benzodiazepines. It is possible that zolpidem abandons its selectivity for the BZ1 receptors and demonstrates all the actions of classic benzodiazepines.
机译:Zolpidem是一种非苯二氮卓催眠药,显示出GABAA受体复合物的调节位点的BZ1(WL)亚型的高亲和力,但经典苯并二氮杂卓(Diazepam,Lorazepam)在WL和W>上具有非特异性亲和力曲线2个GabaA受体的亚型。因此,Zolpidem被认为比苯并二氮杂卓更安全。我们提出了五种患者,随后,癫痫发作,急性精神病和口服障碍症,这些患者开发了Zolpidem。与Zolpidem有关系,很少报告诸如撤离癫痫发作和戒断谵妄的不利影响。与苯二氮卓类化学无关,Zolpidem被认为具有较少的不利影响,但与苯并二氮杂卓分享药代动力学谱。建议,在处方的非苯二氮卓沉积物和催眠术时,也可以使用正常标准,因为它们作用于同一受体,即苯并二氮杂-Gaba-氯化物复合物。然而,在延长时间延长的推荐剂量高于推荐剂量,唑吡斑的上瘾潜力可能与苯并二氮杂卓的类似剂量相似。 Zolpidem可能对BZ1受体进行选择性,并证明了经典苯二氮卓类动物的所有作用。

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