Haloperidol可以增敏索拉非尼诱导的肝癌细胞铁死亡

目的探讨haloperidol对肝癌细胞铁死亡进程的影响,为肝细胞癌的治疗提供新策略。方法索拉非尼处理肝癌细胞株HepG2,Huh-7,SMMC-7721和PLC/PRF/5,在体外构建铁死亡模型,利用CCK-8实验对细胞活性进行检测;用RT-qPCR实验以及Western-blot实验对SlR的mRNA水平及蛋白水平进行检测;向培养基中同时添加haloperidol和索拉非尼,利用CCK-8实验和克隆形成实验对细胞活性进行检测;最后,利用RT-qPCR实验以及Western-blot实验对铁死亡中相关分子GSH以及GPX4的变化进行进一步的检测。结果索拉非尼处理肝癌细胞株HepG2,Huh-7,SMMC-7721和PLC/PRF/5可以导致细胞铁死亡的发生,并且能够被铁死亡的特异性抑制剂Fer-1挽救;在索拉非尼诱导肝癌细胞发生铁死亡的过程中,SlR的表达升高,并且具有统计学意义;和索拉非尼组进行比较,haloperidol+索拉非尼组的细胞活性进一步降低且具有统计学意义;haloperidol能够进一步促进索拉非尼导致的GSH及GPX4表达减少并且具有统计学意义。结论Haloperidol促进索拉非尼导致的GSH及GPX4表达来促进肝癌细胞铁死亡进程,加快肝癌细胞死亡。

Low dose oral haloperidol does not prolong QTc interval in older acutely hospitalised adults： a subanalysis of a randomised double-blind placebo-controlled study

Background Haloperidol is the most frequently prescribed antipsycbotic for delirium symptoms. The risk of QTc prolongation often raises concerns, although the effect of haloperidol on QTc interval has not yet been investigated in a randomised placebo-controlled fixed-dose study. Methods A subanalysis of a randomised double-blind placebo-controlled study was conducted to evaluate the effect of prophylactic haloperidol 1 mg or placebo 1 mg orally twice-daily （maximum of 14 doses） on QTc interval in patients aged 70 years and over. Bedside, 12-lead ECGs were recorded before, during and after the one-week intervention period. Automatic QTc measurements were ob- tained in addition to manual measurements of QT and RR intervals, blinded for treatment status. Manual measurements were corrected （QTc） using Bazett （QTc-B）, Framingham （QTc-Fa）, Fridericia （QTc-Fi） and Hodges （QTc-H） methods. Mixed model analyses were used to test for differences in longitudinal course of QTc between patients receiving haloperidol and placebo. Results ECG recordings of 72 patients （haloperidol n = 38） were analysed, 45.8% male. Median （range） haloperidol serum concentration on day 4 was 0.71 （0.32-1.82） μg/L （n = 23）. Longitudinal course of mean QTc did not significantly differ between treatment arms for any of the automatic or manually derived QTc values. Conclusions Low dose oral haloperidol did not result in QTc prolongation in older acutely hospitalised patients. Results may not be generalizable to patients with existing ECG abnormalities such as atrial fibrillation.

Successful management of delirium with dexmedetomidine in a patient with haloperidol-induced neuroleptic malignant syndrome:A case report

BACKGROUND We report a case of lorazepam-induced agitated delirium treated with haloperidol,which in turn triggered the onset of neuroleptic malignant syndrome(NMS).The latter condition,a medical emergency,was effectively treated with medical treatment and dexmedetomidine,a versatile and highly selective shortacting alpha-2 adrenergic agonist with sedative-hypnotic and anxiolytic effects.CASE SUMMARY A 65-year-old man with a history of bipolar disorder presented to the emergency department with severe abdominal discomfort after binge eating.During his hospital stay,he received intravenous lorazepam for insomnia.On the next day,he became delirious and was thus treated with seven doses(5 mg each)of haloperidol over a 48 h period.Signs of NMS(hyperthermia,rigidity,myoclonus of upper limbs,impaired consciousness,tachypnea,and dark urine)became apparent and haloperidol was immediately suspended and brisk diuresis was initiated.On intensive care unit admission,he was confused,disoriented,and markedly agitated.Dexmedetomidine infusion was started with the goal of achieving a Richmond Agitation-Sedation Scale score of-1 or 0.NMS was resolved gradually and the patient stabilized,permitting discontinuation of dexmedetomidine after 3 d.CONCLUSION Dexmedetomidine may be clinically helpful for the management of NMS,most likely because of its sympatholytic activity.

Effect of <i>Citrus aurantium</i>L. Essential Oil and Haloperidol on Anxiety in Male Mice

Relationship between sociability and the amount of brain’s dopamine is very well known. In this study, we have examined the effect of Citrus aurantium L. essential oil on anxiety and its interaction with dopaminergic pathways. 70 male mice were assigned into experimental, control, and sham groups. Essential oil of Citrus aurantium L. was injected intraperitonealy at doses of 0.5%, 2.5% and 5% for 5 days. Subcutaneous injection of haloperidol was administered on the fifth day, 30 minutes before the injection of the essential oil. The anxiety-related behavior of mice was then assessed by elevated plus-maze test. The result of this study showed that the injection of Citrus aurantium L. essential oil at doses of 2.5% and 5% increased significantly the time spent in the open arms (OAT) (p < 0.001), also there was a significant increase in the number of entries into the open arms (OAE). Injection of different doses of the essential oil along with haloperidol significantly increased OAT (p < 0.001(. The results demonstrate that the essential oil of Citrus aurantium L. along with haloperidol medication reduces anxiety-related behaviors.

A Comparison Study of the Efficacy of Rapid Titration Quetiapine and Haloperidol in Agitated Adults in an Emergency Setting

Objective: Intramuscular (IM) Benzodiazepines and/or Haloperidol alone or with benzodiazepines are frequently used to treat agitation. Based on emerging literature regarding Quetiapine used for the control of anxiety we examined Quetiapine as a possible alternative in selected cases. Methods: This study was a single-blind randomized study comparing Quetiapine PO (300 mg) with a combination of Haloperidol (5 mg), Benztropine mesylate (2 mg) and lorazepam (2 mg) administered IM to treat agitated patients seeking care in a busy psychiatric emergency setting. Male or female patients (18 - 60), deemed by the attending (admitting) psychiatrist to be indicative of agitated and/or aggressive behavior and had a Positive and Negative Syndrome Score-Excited Component (PANSS-EC), as evaluated by the Research Psychiatrist, and total score equal to or greater than 15. Patients deemed competent were randomized into one of the following treatment groups: Quetiapine 300 or Haloperidol 5 mg, benztropine mesylate, or lorazepam given by the IM route. Two scales, PANSS-EC and CGI-C were used to assess patients in the trial. The primary outcome measure PANSS-EC at 2 hours after administration of the medication. Results: Sixty-eight patients were included in the study. There were no significant treatment group differences in baseline condition. There was no significant difference between the two conditions. There was, however, a significant within-group decrease from baseline condition. Conclusion: Finding no significant differences suggests that in general the two treatments were equivalent. To sum up, Quetiapine 300 mg as a single dose appeared safe and effective in agitated patients treated in an ER. The results were similar to a comparison group receiving an intra-muscular combination of Haloperidol, Lorazepam and Benztropine. This study has significant limitations. The study was single blind and the use of a placebo would have strengthened the design but would be considered unethical. The sample size was relatively small and the group of patients who come to the ER may not be representative of the population of patients who visit across the country. And finally it was a select subgroup who made up the study population and who were probably less severely ill than other subjects who came to our ER.

Treatment of Cannabinoid Hyperemesis Syndrome-Associated Nausea with Haloperidol: A Case Report

Introduction: Because of the rising prevalence of cannabis abuse, cannabinoid hyperemesis syndrome (CHS) was recognized as a new medical diagnosis in 2004. Despite the syndrome’s growing prevalence, many providers are unfamiliar with its diagnosis and treatment, and there is little data to back up clinical knowledge and treatment recommendations. For many years, haloperidol has been widely used as an antiemetic, despite a lack of evidence-based clinical data on efficacy and side effects. We present the case of a female who presented to the emergency room with suspected CHS and was treated with haloperidol. Case: A 34-year-old African-American woman with diabetes and a history of marijuana use presented to the emergency department with refractory nausea and vomiting. Her urine drug screen came back positive for THC, but she denied using marijuana prior to this admission. She stated that she was following her current medication regimen. She denied drinking alcohol and smoking cigarettes. Multiple doses of ondansetron, promethazine, scopolamine, and metoclopramide had no effect on the patient. After two days of treatment with haloperidol 5 mg by mouth every 8 hours, nausea and vomiting subsided. Discussion: Haloperidol was able to control nausea and vomiting in six previous case reports of CHS. However, haloperidol was administered intravenously in five of the reports, and the route of administration was not specified in the sixth. To the best of our knowledge, we are the first to demonstrate the benefit of oral haloperidol for CHS. Conclusion: Although cessation of marijuana use is required for long-term resolution of CHS, our case and six others show the benefit of using IV haloperidol for acute management and oral for relapse prevention. More extensive clinical trials are needed to confirm haloperidol’s therapeutic role in patients presenting with CHS symptoms.

Establishment and Effects of Ginger and Kikyoto of a Haloperidol-Induced Dysphagia Model in Guinea Pigs

Dysphagia induces aspiration and causes aspiration pneumonia. There is no treatment for dysphagia fundamentally. Haloperidol reportedly induces dysphagia. In the present study, we established a haloperidol-induced dysphagia model in guinea pigs, and evaluated the effects of ginger, kikyoto, and a mixture of ginger and kikyoto on swallowing. Swallowing ability was evaluated using behavioral tests, computed tomography (CT), and videofluoroscopic examination of swallowing. To investigate the effect of ginger and kikyoto on swallowing, ginger, kikyoto, or a mixture of ginger and kikyoto was administered orally to guinea pigs with haloperidol-induced dysphagia. Effects of these compounds were evaluated with behavioral tests. Chronic administration of haloperidol reduced the number of swallows, as evaluated by the behavioral test and videofluoroscopic examination of swallowing. In our model, these compounds improved swallowing dysfunction. Our results suggest that this model might be useful in revealing the pathogenesis of dysphagia and evaluating compounds that might improve swallowing.

Endocrine and Metabolic Effects of Hydroethanolic Extract of Solenostemon monostachyus on Haloperidol Induced Hyperprolactinemia

The rapid increase in consumption of herbal remedies worldwide has been stimulated by several factors, including the notion that all herbal products are safe and effective. Hyperprolactinemia is a major cause of infertility, and herbal remedies have been employed locally for treatment. This study was designed to investigate the effects of hydroethanolic extract of Solenostemon monostachyus on the reproductive hormones and metabolic parameters of haloperidol-induced hyperprolactinemic rats. Thirty six female albino rats were divided into 6 groups of 6 in each group. Groups A, B, C, D and E were given increasing doses （2, 3 and 4 mg/kg body weight in five-daily increments） of haloperidol by intramuscular injection for 15 days after which they were treated for another 15 days with either 2.5mg/kg body weight ofbromocriptine （group D only） or 75, 112.5 or 225mg/kg body weight of the extract （groups A, B and C, respectively）. Group F was given distilled water only. After treatment, the animals were sacrificed and blood was taken from each group for plasma analysis of the reproductive hormones and metabolic parameters. The total protein and the lipid profile （total cholesterol and HDL （high-density lipoprotein） and triglycerides were also determined. Phytochemical investigation revealed the presence of saponins, phenols, alkaloids, fiavonoids, and tannins. The result of endocrine investigation showed a dose-dependent, statistically significant reduction in prolactin and testosterone （P 〈 0.05） level by the extract with statistical significant increase （P 〈 0.05） in the levels of the follicle stimulating hormone, LH （luteinizing hormone） and estrogen. There was also a decrease in the levels of the triglycerides and total cholesterol while HDL was increased （P 〉 0.05）. It can be concluded from this study, that hydroethanolic extract has a prolactin reducing activity compared with Bromocriptine and exhibited a corresponding statistical significant difference in other reproductive hormones, with no detectable alteration on metabolic parameters such as＂ albumin, total cholesterol, and high density lipoprotein.

Solid lipid nanoparticles for nose to brain delivery of haloperidol:in vitro drug release and pharmacokinetics evaluation

In the present study,haloperidol(HP)-loaded solid lipid nanoparticles(SLNs)were prepared to enhance the uptake of HP to brain via intranasal(i.n.)delivery.SLNs were prepared by a modified emulsification-diffusion technique and evaluated for particle size,zeta potential,drug entrapment efficiency,in vitro drug release,and stability.All parameters were found to be in an acceptable range.In vitro drug release was found to be 94.1674.78%after 24 h and was fitted to the Higuchi model with a very high correlation coefficient(R2¼0.9941).Pharmacokinetics studies were performed on albino Wistar rats and the concentration of HP in brain and blood was measured by high performance liquid chromatography.The brain/blood ratio at 0.5 h for HP-SLNs i.n.,HP sol.i.n.and HP sol.i.v.was 1.61,0.17 and 0.031,respectively,indicating direct nose-to-brain transport,bypassing the blood-brain barrier.The maximum concentration(Cmax)in brain achieved from i.n.administration of HP-SLNs(329.17720.89 ng/mL,Tmax 2 h)was significantly higher than that achieved after i.v.(76.9577.62 ng/mL,Tmax 1 h),and i.n.(90.1376.28 ng/mL,Tmax 2 h)administration of HP sol.The highest drug-targeting efficiency(2362.43%)and direct transport percentage(95.77%)was found with HP-SLNs as compared to the other formulations.Higher DTE(%)and DTP(%)suggest that HP-SLNs have better brain targeting efficiency as compared to other formulations.

The effects of classic antipsychotic haloperidol plus the extract of Ginkgo biloba on superoxide dismutase in patients with chronic refractory schizophrenia

Objectives To explore the association between schizophrenic symptoms and superoxide dismutase (SOD), and to investigate the effect of classic antipsychotic haloperidol plus the extract of Ginkgo biloba (EGb) on SOD Methods In 54 patients with chronic refractory schizophrenia, 27 were treated with haloperidol plus EGb (group 1), and the rest received haloperidol plus placebo (group 2) Superoxide dismutase (SOD) levels of these patients were measured before and after treatment and compared with the levels of 25 healthy volunteers Therapeutic efficacy was equated with a change in clinical rating scores assessed by standardized measurement tools including the Scale for Assessment of Positive Symptoms (SAPS) and the Scale for Assessment of Negative Symptoms (SANS) Results Patients in group 1 improved significantly as demonstrated by scores from both SAPS and SANS, while those in group 2 only by scores from SANS Assessed by SAPS, the response of patients receiving haloperidol plus EGb was more significant than those receiving haloperidol only SOD levels before treatment in all patients were significantly higher than those in normal controls After treatment, SOD levels decreased significantly in group 1 but not in group 2 In addition, before treatment, SOD levels in all patients correlated significantly with SAPS score The levels of SOD measured before treatment were also correlated with the improvement of patients as measured by SAPS and SANS after 12 weeks Conclusions EGb may enhance the efficacy of classic antipsychotic haloperidol on schizophrenia, especially on positive symptoms It may work through an antioxidant efficacy that is involved in the therapeutic mechanism

Emergency department management of acute agitation in the reproductive age female and pregnancy

BACKGROUND:Agitation is a common presentation within emergent departments(EDs).Agitation during pregnancy should be treated as an obstetric emergency,as the distress may jeopardize both the patient and fetus.The safety of psychotropic medications in the reproductive age female has not been well established.This review aimed to explore a summary of general agitation recommendations with an emphasis on ED management of agitation during pregnancy.METHODS:A literature review was conducted to explore the pathophysiology of acute agitation and devise a preferred treatment plan for ED management of acute agitation in the reproductive age or pregnant female.RESULTS:While nonpharmacological management is preferred,ED visits for agitation often require medical management.Medication should be selected based on the etiology of agitation and the clinical setting to avoid major adverse effects.Adverse effects are common in pregnant females.For mild to moderate agitation in pregnancy,diphenhydramine is an effective sedating agent with minimal adverse effects.In moderate to severe agitation,high-potency typical psychotropics are preferred due to their neutral effects on hemodynamics.Haloperidol has become the most frequently utilized psychotropic for agitation during pregnancy.Second generation psychotropics are often utilized as second-line therapy,including risperidone.Benzodiazepines and ketamine have demonstrated adverse fetal outcomes.CONCLUSION:While randomized control studies cannot be ethically conducted on pregnant patients requiring sedation,animal models and epidemiologic studies have demonstrated the effects of psychotropic medication exposure in utero.As the fetal risk associated with multiple doses of psychotropic medications remains unknown,weighing the risks and benefits of each agent,while utilizing the lowest effective dose remains critical in the treatment of acute agitation within the EDs.

针刺联合氟哌啶醇治疗对儿童多发性抽搐症的效果分析

目的 探究针刺联合氟哌啶醇治疗儿童多发性抽搐症的临床疗效。方法 将92例多发性抽搐症患儿按照随机数字表法分为试验组和对照组各46例,对照组予以氟哌啶醇治疗,试验组在氟哌啶醇基础上加用针刺治疗,两组均连续治疗4周。比较两组治疗前后耶鲁综合抽动严重程度量表(YGTSS)、多巴胺(DA)、5-羟色胺(5-HT),治疗后临床疗效及治疗过程中不良反应。结果 治疗后,两组YGTSS评分、DA、5-HT均降低(P<0.05),试验组均低于对照组(P<0.05);治疗后,试验组临床总有效率高于对照组(P<0.05),不良反应组间比较,差异无统计学意义(P>0.05)。结论 针刺联合氟哌啶醇治疗儿童多发性抽搐症可提高临床总有效率,改善临床症状,降低DA、5-HT等神经递质,治疗安全性较高。

利培酮与氟哌啶醇治疗抽动障碍有效性和安全性的Meta分析

目的 系统评价利培酮与氟哌啶醇治疗抽动障碍的有效性和安全性。方法 检索截至2023年8月在维普数据库、中国知网、万方医学数据库、PubMed、Embase和Cochrane Library发表的关于利培酮(观察组)与氟哌啶醇(对照组)治疗抽动障碍的随机对照试验,进行系统评价和Meta分析。2名研究人员利用Cochrane系统评价手册进行偏倚风险评估,使用Rev Man 5.4软件进行数据分析。结果 共纳入23篇研究,涉及1 599例患者。Meta分析显示,观察组患者治疗后不良反应症状量表评分及锥体外系反应、口干、嗜睡/镇静、静坐不能、便秘及体质量增加发生率均低于对照组(P<0.05或0.01);两组患者治疗总有效率、耶鲁综合抽动严重程度量表评分比较,差异无统计学意义(P>0.05)。结论 利培酮与氟哌啶醇均可有效治疗抽动障碍,改善患儿抽动症状,但利培酮的不良反应发生率较低,安全性更高。

奥氮平口溶膜与肌肉注射氟哌啶醇治疗男性住院精神分裂症患者激越行为的随机对照研究

背景男性精神分裂症患者激越行为对患者自身及社会造成严重影响。非侵入性制剂的给药方式可能有助于快速控制激越行为、改善患者体验,但目前关于奥氮平口溶膜治疗精神分裂症患者激越行为的证据有限。目的比较奥氮平口溶膜与肌肉注射氟哌啶醇对改善男性精神分裂症患者激越行为的效果和安全性,以期为患者激越行为的改善提供参考。方法连续纳入2022年5月—2023年7月在阜阳市第三人民医院男性封闭病房住院治疗的、符合《精神障碍诊断与统计手册(第5版)》(DSM-5)诊断标准、伴激越行为的精神分裂症患者(n=44)为研究对象。采用随机数字表法分为研究组和对照组各22例,研究组接受奥氮平口溶膜10 mg/d治疗,对照组接受肌肉注射氟哌啶醇8 mg/d治疗。于治疗前和用药6 h后,使用阳性和阴性症状量表-兴奋因子(PANSS-EC)和激越-镇静评估量表(ACES)评定患者激越行为严重程度,并根据PANSS-EC评分减分率,计算治疗应答率;于用药6 h后,使用锥体外系副反应量表(RSESE)和静坐不能评定量表(BARS)评定药物副反应。结果用药6 h后,两组PANSS-EC评分和ACES评分比较,差异均无统计学意义(F=0.039、0.082,P均>0.05);两组治疗应答率比较,差异无统计学意义(χ^(2)=0.419,P=0.517);研究组不良反应发生率低于对照组,差异有统计学意义(P=0.031)。两组BARS评分比较,差异无统计学意义(t=0.587,P=0.561);研究组RSESE评分低于对照组,差异有统计学意义(t=-7.367,P<0.01)。结论奥氮平口溶膜和肌肉注射氟哌啶醇治疗男性精神分裂症患者激越症状的效果相当,且奥氮平口溶膜的安全性优于肌肉注射氟哌啶醇。

多巴胺对长爪沙鼠贮食行为的影响

长爪沙鼠的贮食行为具有高低二型性。禁食诱导的贮食行为可能与中脑多巴胺(Dopamine,DA)系统有关,但尚乏证据。本文通过Fos标记相关脑区的活性,酪氨酸羟化酶(TH)标记DA神经元,以免疫组化方法观察对高贮食组长爪沙鼠腹腔注射DA拮抗剂haloperidol(1 mg/kg)和对低贮食组长爪沙鼠腹腔注射DA激动剂apomorphine(0.3 mg/kg)的行为和神经变化,验证中枢DA对贮食行为的调节。结果显示,haloperidol抑制了禁食诱导的沙鼠的贮食行为,这种抑制刺激了伏隔核和尾壳核Fos-ir阳性细胞表达,但却降低了黑质区Fos-ir和Fos-ir/TH-ir的细胞表达。Apomorphine增加了禁食诱导的沙鼠的贮食行为,降低伏隔核和尾壳核Fos-ir阳性细胞表达。这些结果表明,中脑DA系统参与调节了禁食条件下长爪沙鼠的贮食行为。

九味熄风颗粒与氟哌啶醇治疗抽动障碍的对照研究

目的比较九味熄风颗粒与氟哌啶醇治疗抽动障碍的临床疗效和安全性。方法将82例门诊治疗抽动症患者随机分成两组各41例,分别给予九味熄风颗粒和氟哌啶醇治疗,疗程6周,在治疗前及治疗后第6、12周末分别采用《耶鲁抽动症整体严重程度量表》(YGTSS)及《副作用量表》(TESS)进行疗效和副反应评估。结果治疗第6周、第12周末九味熄风颗粒组和氟哌啶醇组抽动评分明显降低(P﹤0.05或0.01),九味熄风颗粒组不良反应较氟哌啶醇组少(P﹤0.01)。结论九味熄风颗粒治疗抽动症疗效显著,且安全性好。

碘化N-正丁基氟哌啶醇对大鼠心肌缺血再灌注不同时间肌浆网钙泵活性的影响

碘化N-正丁基氟哌啶醇（N-n-butyl haloperidol iodide,F2）是我课题组合成的一个新化合物（专利号：ZL96119098．1）。以往一系列研究表明，F2可以改善心肌缺血再灌注（ischemia／reperfusion，I／R）造成的血流动力学变化和酶学变化、缩小心肌梗死面积、减轻再灌注心肌组织炎症，对心肌I/R损伤具有全面的保护作用。

喹硫平和氟哌啶醇治疗精神分裂症急性期兴奋激越的多中心随机对照研究

目的:评价喹硫平治疗中国精神分裂症患者急性期兴奋激越的疗效和安全性。方法:本研究为多中心随机对照研究。选取80例符合国际疾病与相关健康问题分类第十版(ICD-10)精神分裂症诊断标准并处于急性兴奋激越状态的患者,按1∶1随机分为喹硫平组(n=40)和氟哌啶醇组(n=40),接受28天的喹硫平或氟哌啶醇治疗。入组时和治疗第1、3、7、10、14、28天进行临床评估,采用阳性与阴性症状量表(PANSS)和总体印象量表中的疾病严重程度(CGI-SI)评估临床症状,并采用PANSS兴奋因子(PANSS-EC)的减分值以及起效时间(PANSS-EC减分率达20%的时间)为主要疗效指标,Simpson-Angus类帕金森综合征量表(SAS)评定锥体外系不良反应。每次临床评估时记录生命体征和服药情况,基线和治疗第28天进行体格检查及血、尿、血生化常规,血清催乳素,心电图等实验室检查。结果:治疗第28天,喹硫平组剂量为(672.9±88.3)mg,氟哌啶醇组剂量为(11.5±3.2)mg。喹硫平组和氟哌啶醇组PANSS-EC评分随着治疗时间的延长逐渐降低,治疗第1天两组均12.5%起效,治疗第7天起效率分别达到82.5%和75.0%。治疗第28天,两组PANSS、CGI-SI量表得分差异无统计学意义,喹硫平组的不良事件发生率(40.0%vs.87.5%)、SAS评分[(0.2±0.8)vs.(1.5±2.2)]和泌乳素水平[(375.0±388.2)μIU/mL vs.(1526.5±1300.6)μIU/mL]均低于氟哌啶醇组(均P<0.05)。喹硫平组的心电图QT间期治疗前后无明显变化,氟哌啶醇组则从(351.8±46.1)ms增加至(374.3±27.5)ms(P<0.05)。结论:喹硫平单药治疗精神分裂症急性期兴奋激越症状起效快速、疗效充分,安全性高、耐受性好。

氟哌啶醇与奥氮平治疗精神分裂症疗效和安全性的随机对照研究

目的比较氟哌啶醇与奥氮平治疗精神分裂症的疗效及安全性。方法将符合精神分裂症诊断标准的住院患者按照1:2比例随机分为氟哌啶醇(n=120)和奥氮平治疗组(n=252),进行为期6周的治疗观察;于基线及治疗2、4、6周末评定阳性和阴性症状量表(positive and negative syndrom scale,PANSS),锥体外系副反应量表(rating scale for extrapyramdal side effects,RSESE)、静坐不能评定量表(barnes akathisia rating scale,BARS)和异常不自主运动量表(abnormal involuntary movement scale,AIMS);计算体质量指数(body mass index,BMI);基线及治疗4、6周末测定空腹血糖、血脂和肝功能等指标。结果氟哌啶醇组与奥氮平组基线PANSS总分差异无统计学意义;第6周末氟哌啶醇组PANSS总分低于奥氮平组(53.31±1.64 vs.58.05±1.02),减分率高于后者(60.63±2.86%vs.52.45±1.80%),均P<0.05;两组有效率(66.7%vs.62.7%)差异无统计学意义。第6周末氟哌啶醇组BMI较基线的变化值(0.08±0.20 kg/m2vs.0.91±0.12 kg/m2)、谷丙转氨酶异常病例数比例(16.98%vs.28.07%)均低于奥氮平组(P<0.05);第4周末氟哌啶醇组甘油三酯较基线的变化值低于奥氮平组(0.24±0.12 mmol/L vs.0.57±0.07 mmol/L),P<0.05。氟哌啶醇组锥体外系不良反应发生率(73.3%)明显高于奥氮平组(10.71%),P<0.05。结论在精神分裂症急性期,氟哌啶醇治疗有效率与奥氮平相当,对体重、血脂、转氨酶的影响较小,但锥体外系不良反应发生率较高。

甲磺酸齐拉西酮与氟哌啶醇注射液治疗精神分裂症急性激越症状的对照研究

目的比较甲磺酸齐拉西酮注射液和氟哌啶醇注射液对精神分裂症急性激越症状的疗效和安全性。方法将86例伴急性激越症状的精神分裂症患者分为观察组（n=43）和对照组（n=43）,进行随机单盲临床对照研究,观察组给予注射用甲磺酸齐拉西酮10-20mg/次肌内注射,每日总量不超过40mg;对照组给予氟哌啶醇针剂5-10mg/次肌内注射,每日总量不超过30mg。两组药物根据病情需要4-6h后可重复使用,每日注射不超过3次,疗程3d。于治疗前和治疗后2、6、24、48、72h采用阳性与阴性症状量表兴奋因子（PANSS-EC）评定激越症状,于治疗前、治疗后72h采用阳性和阴性症状量表（PANSS）、临床疗效总评量表-病情严重程度（CGI-SI）评价疗效;采用锥体外系不良反应量表（SAS）、药物不良反应量表（TESS）、实验室检查评价不良反应。结果与治疗前比较,观察组在治疗后2hPANSS-EC评分即显著降低,其他各观察点PANSS总分、PANSS-EC评分及CGI-SI评分均显著下降（P〈0.01）;但观察组和对照组组间差异无统计学意义（P〉0.05）。两组临床总有效率差异无统计学意义（P〉0.05）。两组均未出现严重不良事件,观察组药物不良反应发生率为37.21%,显著低于对照组的53.49%（P〈0.05）。结论注射用甲磺酸齐拉西酮能有效治疗精神分裂症患者急性激越症状,疗效与氟哌啶醇相当,不良反应发生率更低,安全性好。