Zolpidem dependence in an adult with bipolar affective disorder and epilepsy: A case report

Zolpidem is a short-acting non-benzodiazepine hypnotic agent,commonly recommended for short-term treatment of insomnia.Zolpidem has less dependence potential than benzodiazepines.Patients with mental illnesses often have disturbed sleep,for which zolpidem is often prescribed.Long-term use and self-medication(in more than recommended doses)are more likely to cause dependence.We report here a case of bipolar affective disorder with epilepsy,who developed dependence to zolpidem and had severe withdrawal symptoms.The management issues are also discussed with review of the literature.

More Rapid Sleep Onset with Lingual-Spray vs Oral-Tablet Delivery Zolpidem

Insomnia and related sleep disorders (somnipathies) affect a large segment of the population, and result in a significant negative impact on quality of life and reduced or lost productivity. The speed of sleep onset is a critical characteristic of successful pharmacotherapeutic intervention for insomnia. Zolpidem, a non-benzodiazepine benzodiazepine receptor agonist (nBzRA) is widely used to treat insomnia. Although not itself a benzodiazepine (BZD), zolpidem has high binding affinity for the benzodiazepine receptor, which acts as a positive allosteric modulator of the GABAA receptor complex. It therefore increases the neuronal transmembrane influx of Cl- ions, thereby decreasing neuronal excitability and promoting sleep. In this four-way crossover, dose-ranging, multiple-treatment study, a lingual spray formulation of zolpidem was safe and well-tolerated and yielded more rapid pharmacokinetics (mean plasma concentration) and efficacy (visual analog scale and digit symbol substitution test) compared to oral tablets.

Sleep Related Eating Disorder as an Unexpected Effect of Zolpidem

Zolpidem is a sedative-hypnotic drug used to treat in sleep disorders, and it is the most commonly prescribed drug for insomnia. It reduces sleep latency and increases total sleep time. However, some studies have reported that zolpidem might induce sleep related eating disorder (SRED). SRED is characterized by recurrent episodes of compulsive and involuntary eating during night sleep, accompanied by partial consciousness and limited subsequent recall. The pathophysiology of SRED is unknown. Patients with SRED usually suffer from other sleep disorders such as sleepwalking, restless legs syndrome, and obstructive sleep apnea. In this article, we present an overview of case reports on SRED induced by zolpidem.

Comparison of the Melatonin Receptor Agonist Ramelteon and the Non-Benzodiazepine Hypnotic Zolpidem for Nocturia

To examine the efficacy of the melatonin receptor agonist ramelteon for nocturia, it was compared with zolpidem, a conventional non-benzodiazepine hypnotic. A total of 50 patients with nocturia (32 urinations/night) were enrolled. Subjects assigned odd numbers or even numbers were respectively prescribed 8 mg of ramelteon (n = 27;mean age: 75 years) or 5 mg of zolpidem (n = 23;mean age: 73 years) once a day before sleeping for 4 weeks. The daytime and nighttime frequencies of urination, as well as the results of global self-assessment by the patients, were compared between the two groups before and after 4 weeks of treatment. Both ramelteon and zolpidem caused a significant decrease of nocturia to about once per night after 4 weeks. The global self-assessment rating at 4 weeks was “good” or “fair” for more patients in the zolpidem group than in the ramelteon group, while the rating was “excellent” or “no change” for more patients in the ramelteon group. There were no serious adverse events in either group. Ramelteon was safe and effective for nocturia, achieving similar results to zolpidem. However, responders and non-responders to ramelteon were more clearly distinguished. Ramelteon might be effective for patients with sleep disturbance and nocturia because of low melatonin levels. Therefore, as diagnostic therapy for identification of nocturia caused by sleep disturbance and melatonin deficiency, ramelteon should be administered to patients who do not respond to alpha-1 antagonists and/or anticholinergic agents.

Zolpidem-Induced Narcolepsy, Faint, Seizure or Coma? A Case Report

Zolpidem, as an imidazopyridine agent, is a widely prescribed drug among practitioners for short-term treatment of insomnia. Nevertheless, there have been a number of cases associated with the adverse effects of the stated drug recently. Many cases of serious complications induced by high dose of zolpidem have been reported. Further to the existing reports of adverse reactions to zolpidem, throughout the current manuscript, another case of zolpidem-induced loss of consciousness is going to be presented. The case had taken 100 mg of zolpidem and afterwards, went into an unknown status of narcolepsy, faint, seizure or transient coma. Overdosing zolpidem and being affected by its central effects, he performed risky actions such as cooking by a gas oven and eating meal while intoxicated. The current case suggests that zolpidem overdose might contribute to loss of consciousness and exhibition of high-risk behaviors.

Effect of CYP3A4*18 genotype on the pharmacokinetics of zolpidem in healthy Chinese Hui subjects

In the present study, we aimed to investigate the effect of CYP3A4＊ 18 genotype on the pharmacokinetics of zolpidem in healthy Chinese Hui volunteers. Blood samples were collected from volunteers for CYP3A4 genotyping using a polymerase chain reaction-restriction fragment length polymorphism （PCR-RFLP） assay. A pharmacokinetic study was then carried out in three groups with CYP3A4＊1/＊1 （n = 6）, CYP3A4＊1/＊18 （n = 6） and CYP3A4＊18/＊18 （n = 6） genotypes. Plasma levels of zolpidem were determined by HPLC-FLD method before and after a single oral dose of 10 mg zolpidem tartrate tablet. Significant differences were observed in the pharmacokinetic parameters of zolpidem among the three genotype groups （P〈0.05）. Compared with the CYP3A4＊1/＊1 group, the Cm,x of zolpidem in ＊1/＊18 and ＊18/＊18 groups （mean, 95% CI） was 0.89 （0.65-1.12） and 0.57 （0.47-0.66）, respectively, and the AUC0-1 in the ＊1/＊18 and ＊18/＊18 groups （mean, 95% CI） was 0.74 （0.22-1.26） and 0.61 （0.24-0.98）, respectively. There was a significant trend towards lower Cmax and AUC0-1 values of zolpidem in individuals with more CYP3A＊ 18 alleles, suggesting a gene-dosage effect. The study demonstrated that the CYP3A4＊ 18 allele played an important role in the pharmacokinetics of the zolpidem after oral administration.

长期服用唑吡坦治疗失眠对认知功能损伤机制的研究进展

非苯二氮䓬类药物(唑吡坦)适用于失眠症的短期治疗,长期大剂量使用可导致严重的不良反应。主要的不良反应包括头晕、头疼、跌倒等,严重的可能出现认知功能下降、行为异常,还有药物的耐受性、依赖性、反跳现象和戒断症状等,导致停药困难。分别从唑吡坦的作用机制、不良反应、耐受性、特殊用药等方面进行综述,阐述唑吡坦对认知功能的损伤机制,旨在为探讨长期使用唑吡坦的慢性睡眠障碍患者如何避免认知功能下降提供借鉴。

加味柴平汤联合酒石酸唑吡坦片治疗肝郁脾虚夹湿证失眠临床研究

目的:观察加味柴平汤联合酒石酸唑吡坦片治疗肝郁脾虚夹湿证失眠的临床疗效。方法:选取70例肝郁脾虚夹湿证失眠患者为研究对象,按随机数字表法分为观察组与对照组各35例。对照组给予口服酒石酸唑吡坦片治疗,观察组在对照组治疗方案的基础上予加味柴平汤治疗。治疗1个月后评价临床疗效,观察比较治疗前后中医证候评分变化、匹茨堡睡眠质量指数(PSQI)评分变化及失眠严重程度指数(ISI)评分变化。结果:有4例患者因未能完成疗程服用而脱落,最终纳入统计:观察组33例,对照组33例。治疗后,中医证候评分疗效总有效率观察组87.9%,对照组66.7%,2组比较,差异有统计学意义(P<0.05);2组情志抑郁、脘腹胀满、倦怠乏力、恶心呕吐、便溏不爽、食少纳呆、善太息、胸胁胀满、口中黏腻等中医证候评分均较治疗前降低,差异均有统计学意义(P<0.05),且观察组上述中医证候评分均低于对照组,差异均有统计学意义(P<0.05)。治疗后,PSQI疗效观察组总有效率90.9%,对照组81.8%,2组比较,差异有统计学意义(P<0.05);治疗后,2组PSQI总评分均较治疗前降低,且观察组PSQI总评分低于对照组,差异均有统计学意义(P<0.05)。治疗后,2组睡眠质量、入睡时间、睡眠时间、睡眠障碍、日间功能障碍、睡眠效率评分均较治疗前降低,且观察组睡眠时间、日间功能障碍评分均低于对照组,差异均有统计学意义(P<0.05)。治疗后,2组ISI评分均较治疗前降低,且观察组ISI评分低于对照组,差异均有统计学意义(P<0.05)。结论:加味柴平汤联合酒石酸唑吡坦片治疗有利于改善肝郁脾虚夹湿证失眠的临床症状,从而提高睡眠质量,临床疗效良好。

唑吡坦对低压低氧致失眠模型小鼠的镇静催眠作用

目的研究唑吡坦的镇静催眠作用及对丘脑和下丘脑氨基酸类神经递质含量的影响。方法模拟海拔5500 m低压低氧环境,通过阈上剂量(50 mg·kg^(-1),ip)戊巴比妥钠诱导小鼠翻正反射消失(LORR)实验建立低压低氧致失眠模型。采用LORR实验观察常压常氧和低压低氧条件下唑吡坦(0.33,1,3,9和27 mg·kg^(-1),ip)与戊巴比妥钠镇静催眠阈下(20 mg·kg^(-1),ip)和阈上剂量的协同效应及唑吡坦(10,13,17,20,23,30和40 mg·kg^(-1),ip)的镇静催眠效应。运用高效液相荧光检测法测定常压常氧和低压低氧条件下给予唑吡坦(10,20和40 mg·kg^(-1),ip)1 h后,小鼠丘脑和下丘脑谷氨酸(Glu)和γ-氨基丁酸(GABA)含量。结果低压低氧处理1 d显著缩短阈上剂量戊巴比妥钠诱导小鼠LORR持续时间(P<0.05)。与常压常氧溶媒组和低压低氧致失眠溶媒组相比,常压常氧唑吡坦9和27 mg·kg^(-1)组和低压低氧致失眠模型+唑吡坦9和27 mg·kg^(-1)组均显著缩短阈下及阈上剂量戊巴比妥钠诱导LORR的潜伏期(P<0.01,P<0.05),同时显著延长LORR持续时间(P<0.01,P<0.05);常压常氧唑吡坦组和低压低氧致失眠模型+唑吡坦组致小鼠LORR的半数有效剂量(ED50)分别为16.21和20.55 mg·kg^(-1)。神经递质水平检测结果表明,与常压常氧溶媒组相比,常压常氧唑吡坦40 mg·kg^(-1)组显著降低丘脑和下丘脑Glu含量及下丘脑Glu/GABA比值(P<0.01,P<0.05);与常压常氧溶媒组相比,低压低氧致失眠模型组小鼠下丘脑Glu含量及Glu/GABA比值显著升高(P<0.01,P<0.05),低压低氧致失眠模型+唑吡坦40 mg·kg^(-1)组显著逆转其升高(P<0.05)。结论在低压低氧条件下,唑吡坦的镇静催眠效应减弱,唑吡坦对下丘脑中Glu和GABA水平的调节可能在其镇静催眠效应中发挥重要作用。

非苯二氮䓬类药物治疗失眠共病睡眠呼吸暂停的临床效果评价研究新进展

失眠共病睡眠呼吸暂停(COMISA)是一种高患病率的临床综合征,其特点是同时伴有失眠和阻塞性睡眠呼吸暂停,且相比单独失眠或睡眠呼吸暂停(OSA)患者,其导致的日间功能和生活质量的损害更为严重。非苯二氮䓬类药物(NBZDs)可改善失眠症状、提高睡眠质量,是治疗失眠的一线用药,但因其可能会增加呼吸暂停低通气指数(AHI)和恶化OSA严重程度而不推荐用于OSA治疗。目前,NBZDs对COMISA的治疗效果尚不明确,还有待深入研究。因此,本文采用系统回顾的方式,整理了OSA和COMISA患者使用NBZDs的相关文献,分析NBZDs对AHI、氧减指数、睡眠质量等多个指标的影响,评价了佐匹克隆、右佐匹克隆、唑吡坦及扎来普隆等药物治疗的临床效果及安全性,旨在为COMISA患者如何合理使用NBZDs提供借鉴。

酒石酸唑吡坦关键中间体的有关物质检测与主要杂质合成酒石酸唑吡坦关键中间体的有关物质检测与主要杂质合成

目的控制酒石酸唑吡坦关键中间体化合物3的质量。方法采用高效液相色谱法检测化合物3中有关物质,色谱柱为Agilent Pursuit 5 C_(18)柱(150 mm×3.9 mm,5μm),流动相为pH 6.0磷酸盐缓冲液-甲醇-乙腈(梯度洗脱),流速为1.2 mL/min,柱温为30℃,检测波长为254nm,进样量为20μL。合成化合物3中的主要杂质,并通过质谱法、核磁共振波谱法对其进行结构确认。结果化合物3的质量浓度在0.0928~556.7689μg/mL范围内与峰面积线性关系良好(r=0.9997,n=5);检测限为1.0 ng,定量限为2.0 ng;精密度、稳定性、重复性试验的结果均符合要求。6批化合物3的纯度均大于90%,均检出有关物质杂质1、杂质2、未知杂质、化合物2,其相对保留时间分别为0.32,1.12,2.23,1.67。以化合物3为原料,合成得到杂质1和杂质2,纯度分别为99.04%和98.72%。结论该方法专属性强、准确度高、稳定性好,可为酒石酸唑吡坦的质量控制提供参考。合成的杂质纯度高,可作为杂质对照品使用。

枣仁安神胶囊联合酒石酸唑吡坦治疗失眠的临床疗效

目的 分析失眠患者使用枣仁安神胶囊联合酒石酸唑吡坦片进行治疗的效果。方法 88例失眠患者作为研究对象,经随机抽样法分为常规组和研究组,每组44例。常规组患者使用酒石酸唑吡坦片治疗,研究组使用枣仁安神胶囊联合酒石酸唑吡坦片治疗。比较两组治疗效果、不良情绪评分、睡眠质量评分、中医证候积分、心理健康状况评分。结果 常规组治疗总有效率为81.82%,研究组治疗总有效率为97.73%;和常规组相比,研究组治疗总有效率更高(P<0.05)。治疗前,两组焦虑、抑郁评分相比无明显差异(P>0.05);常规组治疗后焦虑、抑郁评分分别为(53.73±3.31)、(51.88±2.95)分,研究组治疗后焦虑、抑郁评分分别为(42.03±1.46)、(45.15±0.68)分,治疗后,研究组焦虑、抑郁评分均低于常规组,组间具有明显差异(P<0.05)。治疗前,两组主观睡眠质量、白天功能障碍、睡眠时间、入睡时间、多梦、夜间觉醒评分相比无明显差异(P>0.05);治疗后,常规组主观睡眠质量、白天功能障碍、睡眠时间、入睡时间、多梦、夜间觉醒评分分别为(1.68±0.57)、(1.12±0.28)、(1.22±0.11)、(1.38±0.54)、(1.33±1.21)、(1.45±0.52)分,研究组分别为(1.12±0.24)、(0.75±0.24)、(0.98±0.27)、(0.51±0.16)、(0.61±0.04)、(0.94±0.41)分,研究组主观睡眠质量、白天功能障碍、睡眠时间、入睡时间、多梦、夜间觉醒评分均低于常规组(P<0.05)。治疗前,两组中医证候积分、心理健康状况评分相比无明显差异(P>0.05);治疗后,研究组中医证候积分、心理健康状况评分分别为(0.51±0.44)、(138.67±16.14)分,常规组分别为(1.39±0.47)、(165.54±14.58)分,研究组均低于常规组(P<0.05)。结论 失眠患者使用枣仁安神胶囊联合酒石酸唑吡坦片进行治疗,可以改善患者睡眠质量,减少患者不良情绪,和单用酒石酸唑吡坦片相比,疗效更高,临床应用价值较高。

CYP2C19基因多态性对唑吡坦治疗缺血性脑卒中后失眠症的血药浓度及疗效影响

目的:探讨CYP2C19基因多态性对唑吡坦治疗缺血性脑卒中后失眠症的血药浓度及疗效的影响。方法:选取2021年10月至2023年12月东莞市万江医院收治的缺血性脑卒中后失眠症患者60例作为研究对象,按照随机数字表法分为对照组和观察组,每组30例。研究对象均予唑吡坦治疗,对照组采取经验性用药,观察组根据CYP2C19基因多态性检测结果个体化用药。对比分析2组的血药浓度、疗效情况以及治疗前后睡眠障碍评定量表(SDRS)评分。结果:2组的血药浓度比较,差异无统计学意义(P>0.05)。观察组患者治疗后SDRS评分低于对照组,差异有统计学意义(P<0.05)。观察组的总有效率高于对照组,差异有统计学意义(P<0.05)。结论:CYP2C19基因多态性检测在指导唑吡坦治疗缺血性脑卒中后失眠症的个体化用药方面有着良好的价值。

Comparative pharmacokinetics of zolpidem tartrate in five ethnic populations of China

The objective of this study was to evaluate the difference in the pharmacokinetics of zolpidem tatrate in subjects from five Chinese ethnicities(Han,Mongolian,Uigur,Korean and Hui).Healthy subjects(10 Hans,10 Mongolians,10 Uigurs,10 Koreans and 9 Huis)were recruited and each received a 10 mg tablet-dose of zolpidem tatrate.A total of 12 plasma samples were collected over a 12 h period after administration.The concentrations of zolpidem in plasma were determined by an HPLC-FLU method,after which the pharmacokinetic parameters were determined using DAS 2.0 software and analyzed by SPSS 16.0 software.After normalization by weight,no differences were noted in the pharmacokinetic parameters of zolpidem tatrate among the five ethnic groups(P>0.05).However,there were statistically significant differences between males and females for the pharmacokinetic parameters(P<0.05).The metabolism of zolpidem tatrate in males was faster than in females.Results indicate that ethnicity has no significant impact on the pharmacokinetics of zolpidem tatrate after a single oral dose in healthy Chinese subjects.However,an effect of gender on the pharmacokinetics of zolpidem tatrate can be noted.

脑电生物反馈联合酒石酸唑吡坦片治疗急性缺血性卒中后睡眠障碍临床观察

目的:观察脑电生物反馈联合酒石酸唑吡坦片治疗急性缺血性卒中后睡眠障碍的临床疗效。方法:选取2022年2月1日至2023年8月31日福建省老年医院神经内科收治的急性缺血性卒中后睡眠障碍患者77例作为研究对象进行回顾性调查。根据治疗方案分为对照组(n=42)和观察组(n=35),对照组采用酒石酸唑吡坦片口服治疗,观察组采用脑电生物反馈联合酒石酸唑吡坦片治疗。2组均治疗2周,比较2组干预前后匹兹堡睡眠质量指数(PSQI)评分及睡眠时间、觉醒次数及觉醒时间,并评定临床疗效。结果:治疗后2组PSQI评分、睡眠时间、觉醒次数及觉醒时间均较本组治疗前改善(P<0.05),且观察组治疗后改善优于对照组(P<0.05);观察组总有效率高于对照组(P<0.05)。结论:脑电生物反馈联合酒石酸唑吡坦片显著改善急性缺血性卒中后睡眠质量,疗效肯定。

坤泰胶囊联合唑吡坦治疗肾虚肝郁型更年期综合征睡眠障碍的效果研究

目的探究肾虚肝郁型更年期综合征睡眠障碍患者应用坤泰胶囊联合唑吡坦治疗的效果。方法选取60例肾虚肝郁型更年期综合征睡眠障碍患者,按照随机数字表法分为对照组(30例,予以唑吡坦治疗)与治疗组(30例,予以唑吡坦联合坤泰胶囊治疗)。比较两组治疗效果、睡眠质量、检测指标及不良反应发生情况。结果治疗组总有效率96.67%高于对照组的76.67%(P<0.05)。治疗后治疗组匹兹堡睡眠质量指数量表(PSQI)评分低于对照组(P<0.05)。治疗组雌二醇(E_(2))水平高于对照组,卵泡刺激素(FSH)、促黄体生成素(LH)水平低于对照组(P<0.05)。两组不良反应发生率比较,差异无统计学意义(P>0.05)。结论肾虚肝郁型更年期综合征睡眠障碍患者应用坤泰胶囊联合唑吡坦治疗效果突出,能够改善睡眠质量,调节性激素水平,安全系数高。

柴胡加龙骨牡蛎汤化裁对失眠小鼠的神经调节机制探索

目的研究柴胡加龙骨牡蛎汤化裁方对失眠小鼠脑干中5-羟色胺(5-hydroxytryptamine,5-HT)、5-羟基吲哚乙酸(5-hydroxyindole acetic acid,5-HIAA)、γ-氨基丁酸(γ-aminobutanoic acid,GABA)含量的影响。方法选取40只雄性小鼠随机分为模型组、柴胡组(柴胡加龙骨牡蛎汤治疗)、唑吡坦组(酒石酸唑吡坦片治疗)、空白对照组,每组10只。模型组、柴胡组、唑吡坦组(合称实验组)小鼠腹腔注射对氯苯丙氨酸造模,对照组腹腔注射生理盐水,共3天。造模成功后,对各组小鼠进行药物灌胃,柴胡组予柴胡加龙骨牡蛎汤化裁颗粒,唑吡坦组予酒石酸唑吡坦片,模型组和空白对照组予生理盐水。干预7天后取小鼠脑干,通过酶联免疫吸附法分别对5-HT、5-HIAA、GABA含量进行测定。结果模型组小鼠脑干中5-HT、5-HIAA、GABA的含量较空白对照组明显下降(P<0.05),说明造模成功;柴胡组与唑吡坦组小鼠脑干中5-HT、5-HIAA、GABA含量均高于模型组(P<0.05),但低于空白对照组(P<0.05);柴胡组与唑吡坦组小鼠脑干中5-HT、5-HIAA、GABA含量无明显统计学差异(P>0.05)。结论柴胡加龙骨牡蛎汤化裁方可改善失眠小鼠的睡眠质量,可能与其能够促进小鼠脑干中5-HT、5-HIAA、GABA的分泌有关,其短期疗效与酒石酸唑吡坦相当。