Pumpkin seed ethanolic extract protects against escitalopram-induced reproductive toxicity in male mice

Objective:To investigate the protective role of pumpkin seed ethanolic extract against escitalopram-induced reproductive toxicity in male mice.Methods:Swiss albino male mice were randomly divided into five groups with six mice in each group.Group Ⅰreceived normal water orally,Group Ⅱ,Ⅲ,Ⅳand Ⅴreceived escitalopram oxalate(10 mg/kg),pumpkin seed extract(300 mg/kg)plus escitalopram oxalate(10 mg/kg),escitalopram oxalate(20 mg/kg),and pumpkin seed extract(300 mg/kg)plus escitalopram oxalate(20 mg/kg),respectively.All test doses were continuously administered orally once daily per animal body weight for 30 days and 60 days.Body weight and sexual organ weight were evaluated on day 31 and 61.Effects of pumpkin seed extract on sperm parameters,biochemical parameters and histology of testis were also investigated.Results:Escitalopram 10 or 20 mg/kg caused reproductive toxicity in male mice after 30 and 60 days of treatment.However,simultaneous administration of escitalopram oxalate(10 or 20 mg/kg)with pumpkin seed extract(300 mg/kg)attenuated escitalopram-induced testicular toxicity.Significant increase in the body weight and relative organ weight was observed.Sperm count,sperm motility and viability significantly increased(P<0.05).The histopathological alterations caused by escitalopram was also ameliorated.Conclusions:Ethanolic extract of pumpkin seeds(300 mg/kg body weight)protects again reproductive toxicity induced by escitalopram.Therefore,dietary intake of pumpkin seed extract might be useful for male patients who expose to antidepressant drug due to depression.

Clinical efficacy and safety of Guipi decoction combined with escitalopram oxalate tablets in patients with depression

BACKGROUND Depression is a widespread mental health condition that requires effective treatment.In the treatment of depression,traditional Chinese medicine(TCM)offers obvious advantages,fewer adverse reactions,and a lower recurrence rate.AIM To evaluate the clinical benefits of Guipi decoction combined with escitalopram oxalate tablets for individuals with depression.METHODS In total,80 patients diagnosed as having depression were enrolled in the study and divided into either an experimental group or a control group.All of the patients were orally administered escitalopram oxalate tablets.Additionally,the experimental group received Jiajian Guipi decoction and reduced Governor vessel fumigation over 4 wk.TCM syndrome scores,Hamilton depression rating scale(HAM-D)scores,self-rating depression scale(SDS)scores,and Pittsburgh sleep quality index scores were measured for the two groups and compared before and after the treatment.The two groups were monitored for any adverse reactions.RESULTS After 4 wk of treatment,both groups exhibited a significant reduction in TCM syndrome scores compared with their pre-treatment scores(P<0.05).However,the experimental group exhibited significantly lower TCM syndrome scores than the control group(P<0.05).Similarly,the post-treatment SDS and HAM-D-24 scores were significantly lower in both groups than the pre-treatment scores(P<0.05),with the experimental group exhibiting lower scores than the control group(P<0.05).The total treatment efficiency was significantly better in the experimental group(97.14%)than in the control group(77.78%)(P<0.05).Furthermore,after 4 wk of treatment,the Pittsburgh sleep quality index scores for both groups were significantly lower than those before the treatment(P<0.05),with the experimental group exhibiting lower scores than the control group(P<0.05).The incidence of adverse reactions was significantly lower in the experimental group than in the control group(P<0.05).CONCLUSION The combination of Guipi decoction and escitalopram oxalate tablets was found to be an effective and safe treatment for depression.This combination could reduce TCM syndrome scores,improve depressive symptoms,and enhance sleep quality.

Pilot study of genome-wide DNA methylation and gene expression for treatment response to escitalopram in panic disorder

BACKGROUND Antidepressants,particularly selective serotonin reuptake inhibitors,are currently considered the first-line treatment for panic disorder(PD).However,little is known about the relationship between the biomarkers that may predict better treatment.AIM To compare genome-wide methylation and gene expression patterns between responsive and non-responsive patients with PD after 4 wk of escitalopram treatment.METHODS Thirty patients with PD were enrolled in this study(responders=13;nonresponders=17).All patients were assessed using the PD Severity Scale-Chinese version before and after treatment.The Illumina Infinium MethylationEPIC(850k)BeadChip for genome-wide methylation screening and mRNA sequencing was used in all patients with PD.RESULTS A total of 701 differentially methylated positions(DMPs)were found between responders and non-responders(|Δβ|≥0.06,q<0.05),and the hyper-and hypomethylated CpG sites were 511(72.9%)and 190(27.1%),respectively.Relative to non-responders,there were 59 differential transcripts,of which 20 were downregulated and 39 were upregulated(q<0.05).However,no differen tially expressed genes were identified by mRNA sequencing after correcting for multiple testing(|log2(FC)|>1,q>0.05).CONCLUSION This preliminary study showed that DMPs might be associated with the treatment response to escitalopram in PD;however,these DMPs need to be verified in large samples.

Neuroprotective Effect of Escitalopram Oxalate in Rats with Chronic Hypoperfusion

Summary： The neuroproteetive effects of escitalopram oxalate in rats with chronic hypoperfusion and the possible mechanism were explored. Chronic hypoperfusion （2-VO） model was prepared and given escitalopram oxalate （experimental group） or PBS （control group） after 6 weeks. Eight weeks after the operation, Morris water maze test was carried out to evaluate the learning and memory ability of the rats. The cell proliferation, three-dimensional vascular distribution, cell morphological changes in ischemic area and the plasma vascular endothelial growth factor （VEGF） were detected to explore the possible mechanisms. （1） Morris water maze test showed that the escape latency in the experimental group was significantly shorter than in the control group, while the first quadrant swimming time in the experi- mental group was significantly longer than the control group （both P〈0.01）. （2） Cerebrovascular confo- cal detection results showed that the inside diameter of capillaries was significantly less in the experi- mental group than in the control group; the vascular density was significantly increased in the experi- mental group and the total area of capillaries was also significantly increased in the experimental group as compared with the control group. （3） There was statistically significant difference in BrdU-positive cells in the ischemic brain tissue between the experimental group and the control group （P=0.003〈0.01）. （4） VEGF concentrations in the plasma and the ischemic area were higher in the experimental group than in the control group （P〈0.05）. It was concluded that escitalopram oxalate could significantly im- prove the learning and memory ability of the rats with chronic cerebral ischemia probably by the VEGF-mediated angiogenesis.

Escitalopram-induced liver injury: A case report and review of literature

BACKGROUND Depression is a growing public health problem that affects over 350 million people globally and accounts for approximately 7.5%of healthy years lost due to disability.Escitalopram,one of the first-line medications for the treatment of depression,is a selective serotonin reuptake inhibitor and one of the most commonly prescribed antidepressant medications worldwide.Although thought to be generally safe and with minimal drug-drug interactions,we herein present an unusual case of cholestatic liver injury,likely secondary to escitalopram initiation.CASE SUMMARY A 56-year-old Chinese lady presented with fever and cholestatic liver injury two weeks after initiation of escitalopram for the treatment of psychotic depression.Physical examination was unremarkable.Further investigations,including a computed tomography scan of the abdomen and pelvis and tests for hepatitis A,B and C and for autoimmune liver disease were unyielding.Hence,a diagnosis of escitalopram-induced liver injury was made.Upon stopping escitalopram,repeat liver function tests showed downtrending liver enzymes with eventual normalization of serum aspartate aminotransferase and alanine aminotransferase one-week post-discharge.CONCLUSION Clinicians should be aware of the possibility of escitalopram-induced liver injury when initiating depressed patients on antidepressant treatment.This requires extra vigilance as most patients may remain asymptomatic.Measurement of liver function tests could be considered after initiation of antidepressant treatment,especially in patients with pre-existing liver disease.

Effect of escitalopram on cognitive function in depressionA mismatch negativity potentials study

We detected the event-related potential mismatch negativity （MMN） of 30 depression patients and compared to 30 age,gender,and education-matched healthy controls.Results showed that amplitudes of frequency and duration MMN were lower in depression patients compared with control patients,indicating abnormality in auditory processing （i.e.,cognitive impairment）.Following escitalopram treatment for 8 weeks,the amplitudes of frequency and duration MMN were significantly increased and Hamilton Rating Scale for Depression scores were significantly decreased in depression patients.These data suggest that escitalopram can improve cognitive function of patients with depression.Further,MMN may be a useful tool for evaluating cognitive function and treatment effects.

The Efficacy of Escitalopram Combined with Olanzapine in Depression:A Systematic Review and Meta-analysis

Background:Depression will become the second most common disease after coronary heart disease(CHD).Escitalopram and olanzapine are commonly used to treat depression.Some studies indicated that escitalopram combined with olanzapine is effective in treating depression,however,there is no evidence to support these results.Our objective was to study the efficacy of escitalopram combined with olanzapine on depression by conducting a systematic review and meta analysis,and to provide reference for doctors.Methods:Relevant evidence were searched from PubMed,SinoMed,the Cochrane Library,Web of Science,Embase,China Knowledge Resource Integrated(CNKI),Wanfang Data Knowledge Service Platform databases(WANFANG)and VIP dating from inception to July 2020.The randomized controlled trials(RCTs)of escitalopram and olanzapine for the treatment of depression was obtained.According to inclusion and exclusion criteria,two researches(Sun Wu and Wang Zhe)independently screened the literature,extracted data,and evaluated the quality of included studies.Rev Man 5.3 software was used to conduct statistical analyze.Results:A total of 39 studies involving 3,267 patients were identified.These studies were finally included into the meta-analysis.Pooled results showed that there was a significant difference in efficiency(RR=1.18,95%CI:1.14 to 1.12,P<0.00001),HAMD(MD=-4.54,95%CI:-5.09 to-3.99,P<0.00001),and HAMA(MD=-3.94,95%CI:-5.57 to-2.12,P<0.0001).There was no significant difference in adverse reactions(MD=0.07,95%CI-0.03 to 0.17,P=0.19).Heterogeneity test showed that due to the high heterogeneity of HAMD(P<0.00001,12=86%)and HAMA(P<0.00001,I2=91%),after removing the items with high heterogeneity,there were also statistically significant in HAMD(MD=-5.22,95%CI:-5.53 to-4.91,P<0.00001)and HAMA(MD=-5.46,95%CI:-6.15 to-4.77,P<0.00001).Conclusion:Based on this study,the combination of escitalopram and olanzapine was more effective in treating depression than the control group.It is suggested that clinical and scientific researchers carry out more high-quality,large-sample,multi-center RCTs to provide more evidence-based medical evidence for the future study of escitalopram combined with olanzapine in the treatment of depression.

Relief of hot flashes with escitalopram in non-depressed menopausal women in Japan: Results of a retrospective analysis

Purpose: Hormone therapy (estrogen with or without progestin) remains the gold standard treatment for hot flashes in menopausal women, but concerns for the risk of hormone therapy have resulted in its decline and a demand for nonhormonal treatments with demonstrated efficacy for hot flashes. Aim of this study was to examine the efficacy of selective serotonin reuptake inhibitor escitalopram on hot flashes in a healthy sample of non-depressant menopausal women in Japan. Methods: We retrospectively analyzed the medical records of 11 menopausal patients with hot flashes, who received escitalopram (10 mg daily) for 2 weeks between March and August 2012. Hot flashes severities and scores were recorded on a scale of 0 to 10 points, at beginning and end of 2 weeks treatment. Results: At 2 weeks of therapy, 9 of 11 patients reported significant decreases in hot flash frequency and severity, but the remission of the symptom was not observed in 2 patients. Speed of relief from hot flashes was rapid (within one week). Conclusions: Escitalopram 10 mg/day may be a prompt and effective option for treating hot flashes in menopausal women who do not want to use hormone replacement therapy.

Escitalopram-induced hepatitis:A case report

BACKGROUND The antidepressant escitalopram is widely prescribed for the treatment of depression.It is generally well-tolerated,and cholestasis is not mentioned in its summary of product characteristics(Sm PC).We present a case of cholestatic and cytolysis liver injury due to escitalopram and a Vigi Base?study.CASE SUMMARY A 68-year-old man was admitted to our emergency unit due to clinical jaundice associated with hepatitis,pruritus and dark urine.We tested the patient for the most common etiologies of jaundice,including hemolysis,viral hepatitis,cirrhosis,carcinoma,cholangitis,cholelithiasis and intrahepatic or extrahepatic obstruction.The etiological study was negative,and an adverse drug reaction was the sole possible explanation.The patient was receiving treatment with escitalopram.Two days after its withdrawal,pruritus was resolved.Ten days after withdrawal,clinical jaundice disappeared.It took a month and three weeks after withdrawal for the patient to have normalized liver function tests.To our knowledge,this is the first reported case of cholestasis where treatment with escitalopram was the only possible cause,with a highly probable causality.In addition,we determined whether escitalopram is associated with hepatotoxicity and cholestasis by performing a disproportionality analysis.All cases of hepatobiliary disorders induced by escitalopram and reported in the World Health Organization pharmacovigilance database(Vigi Base?)were analyzed to characterize this toxicity.We found that patients treated with escitalopram had an increased risk of hepatitis[odds ratio(OR)=1.938(1.186-3.166)]and cholestasis[OR=1.866(1.279-2.724)][OR(95%confidence interval)].The median duration between the introduction of escitalopram and the occurrence of acute hepatitis and/or cholestasis was ten days+/-seven days.CONCLUSION Although extremely rare,this case report,the review of the literature and the pharmacovigilance update confirm that escitalopram can cause drug-induced hepatotoxicity and cholestasis,generally within a week after initiation.Thus,escitalopram should be withdrawn immediately if an iatrogenic cause cannot be excluded.If its responsibility is ascertained,escitalopram should be consequently contraindicated.In addition,serotoninergic antidepressants in patients with nonsevere depression are ineffective and harmful.Finally,the Sm PC of escitalopram should be updated to alert for this risk and give clear clinical guidelines.

坦索罗辛联合艾司西酞普兰治疗慢性骨盆疼痛综合征的疗效观察

目的分析坦索罗辛联合艾司西酞普兰治疗慢性骨盆疼痛综合征的临床疗效、症状改善和炎症水平的影响。方法选取2022年1月至2023年1月收治的慢性骨盆疼痛患者120例作为研究对象(参考Kendall样本量估计方法,样本量:观察变量的10~20倍,预计估算量:60~120个),随机数表法分为对照组和观察组,每组60例。对照组给予坦索罗辛治疗,观察组给予坦索罗辛联合艾司西酞普兰治疗,疗程均为2个月。比较2组患者治疗前、后的排尿症状、炎性因子水平、临床指标和症状积分变化情况,对比2组患者的不良反应发生情况。结果观察组患者的尿频尿急、尿后滴沥、排尿疼痛评分和总积分均低于对照组(P<0.05);观察组治愈率显著高于对照组(P<0.05);观察组白细胞计数(WBC)、白介素-1β(IL-1β)、干扰素-α(INF-α)均低于对照组,平均尿流率(AFR)、白细胞介素-2(IL-2)均高于对照组(P<0.05);2组不良反应发生率差异无统计学意义(P>0.05)。结论坦索罗辛联合艾司西酞普兰治疗慢性骨盆疼痛综合征有助于改善临床症状和临床指标、抑制炎性反应,临床疗效较好。

艾司西酞普兰联合焦点解决短程治疗对青少年抑郁患者负性情绪、认知功能的影响

目的分析艾司西酞普兰联合焦点解决短程治疗对青少年抑郁患者负性情绪、认知功能的影响。方法选取2021年12月至2023年6月在杭州市第七人民医院就诊的60例抑郁症青少年患者,根据随机数字表法分为观察组(30例)和对照组(30例)。对照组使用艾司西酞普兰治疗,观察组在对照组治疗的基础上联合焦点解决短程治疗。对比两组患者的临床疗效、负性情绪、认知功能、不良反应。结果治疗后2~6周两组患者健康问卷评分均降低,观察组较对照组更优(均P<0.05);两组的汉密尔顿抑郁量表评分、广泛性焦虑自评量表评分均降低,观察组较对照组更低(均P<0.05);两组的精神状态评定量表评分均上升,观察组较对照组的认知功能更优(均P<0.05)。与对照组相比,观察组的不良反应总发生率更低(P<0.05)。结论艾司西酞普兰联合焦点解决短程治疗不仅可缓解青少年抑郁患者的焦虑和负面情绪,还能提高患者的认知功能,降低不良反应发生率,值得在临床推广应用。

草酸艾司西酞普兰联合复方解郁汤治疗青少年抑郁症的临床疗效分析

目的 探讨草酸艾司西酞普兰联合复方解郁汤治疗青少年抑郁症的临床疗效。方法 选择该院2021年12月—2022年12月期间精神科收治青少年抑郁症患者86例,按照随机数字表法分试验组(43例)和对照组(43例)。所有患者均予以认知行为疗法治疗,对照组予以草酸艾司西酞普兰片,试验组在对照组的基础上联用复方解郁汤治疗。两组均以4周为1个疗程,共治疗2个疗程。对比两组治疗前后脑源性神经营养因子水平、血清炎症因子水平、单胺类神经递质水平、抑郁情况评分、睡眠质量评分、自杀态度评分,观察并评估两组治疗效果及治疗期间不良反应。结果 与治疗前比,治疗后两组BDNF水平较高,IL-1β、IL-6、TNF-α水平降低;与对照组比,治疗后试验组BDNF水平较高,IL-1β、IL-6、TNF-α水平较低(P<0.05)。与治疗前比,治疗后两组NE、5-HT、DA水平升高;与对照组比,治疗后试验组NE、5-HT、DA水平较高(P<0.05)。与治疗前比,治疗后两组HAMA及PSQI评分降低;与对照组比,治疗后试验组HAMA及PSQI评分较低(P<0.05)。试验组临床总有效率较对照组高,差异有统计学意义(P<0.05)。与治疗前比,治疗后两组自杀意念QSA评分较高;与对照组比,治疗后试验组自杀意念QSA评分较高(P<0.05)。两组均未出现严重不良反应,比较差异无统计学意义(P>0.05)。结论 草酸艾司西酞普兰联合复方解郁汤对青少年抑郁症患者的治疗效果显著,能上调脑源性神经营养因子及单胺类神经递质水平,降低血清炎症因子水平,改善睡眠质量及自杀意念,不良反应较少,是一种安全有效的治疗方案。

阿戈美拉汀与草酸艾司西酞普兰联合治疗对抑郁症患者症状及睡眠质量的影响

目的研究阿戈美拉汀与草酸艾司西酞普兰联合治疗对抑郁症患者症状及睡眠质量的影响。方法单纯选取2022年10月—2023年8月泉州市第三医院收治的100例抑郁症患者作为研究对象,采用随机数表法分为两组,每组50例。对照组给予草酸艾司西酞普兰治疗,观察组给予阿戈美拉汀与草酸艾司西酞普兰治疗。对比两组患者不同治疗时间的抑郁症状程度、睡眠质量以及药物不良反应。结果治疗4、8周后,观察组的汉密尔顿抑郁量表(Hamilton Depression Scale,HAMD)评分均低于对照组,差异有统计学意义(P均<0.05)。治疗8周后,观察组匹兹堡睡眠质量指数(Pittsburgh Sleep Quality Index,PSQI)中各个项目(日间功能障碍、催眠药物、入睡时间、睡眠时间、睡眠质量、睡眠效率及睡眠障碍)评分均低于对照组,差异有统计学意义(P均<0.05)。两组患者药物不良反应总发生率比较(12.00%vs 8.00%),差异无统计学意义(χ^(2)=0.444,P=0.504)。结论阿戈美拉汀与草酸艾司西酞普兰联合治疗可更有效减轻抑郁症患者的症状程度,改善患者的睡眠质量,且不会明显造成药物不良反应的发生,安全性相对有保障。

柴胡汤联合草酸艾司西酞普兰对围绝经期抑郁症患者心理弹性和症状及激素水平的影响分析

目的探究柴胡汤联合草酸艾司西酞普兰对围绝经期抑郁症患者心理弹性、症状及激素水平的影响。方法选取2021年6月至2022年11月天津中医药研究院附属医院收治的98例围绝经期抑郁症患者为研究对象,采用随机数字表法分为对照组和观察组,各49例。对照组给予草酸艾司西酞普兰治疗,观察组在对照组基础上给予柴胡汤治疗。2组均连续治疗2个月。比较2组治疗前后心理弹性、症状以及血清激素、5-羟色胺、脑源性神经营养因子(BDNF)水平。结果治疗后,2组心理弹性量表评分、5-羟色胺、BDNF、雌激素水平均高于治疗前,且观察组均高于对照组[81(74,85)分比73(70,77)分、(36.5±3.7)ng/L比(32.2±3.4)ng/L、(18.7±1.9)ng/L比(15.4±1.7)ng/L、(26.3±2.8)ng/L比(22.1±2.4)ng/L](均P<0.05);2组Kupperman评分、汉密尔顿抑郁量表评分、促黄体生成素、卵泡刺激素水平均低于治疗前,且观察组均低于对照组(均P<0.05)。结论柴胡汤联合草酸艾司西酞普兰治疗围绝经期抑郁症可有效改善患者心理弹性水平、缓解症状并降低相关激素水平。

心悦胶囊与艾司西酞普兰联合常规抗心衰治疗对慢性心力衰竭患者“双心”治疗研究

目的 探讨心悦胶囊联合常规抗心衰治疗与艾司西酞普兰联合常规抗心衰治疗在慢性心力衰竭合并焦虑抑郁患者中的有效性及安全性。方法 选取2021年3月—2022年1月在赣南医学院第一附属医院确诊的慢性心力衰竭患者150例,按照简单随机分组方法分为常规治疗组(给予沙库巴曲缬沙坦等药物)、心悦胶囊组、艾司西酞普兰组,每组50例。分别在患者入院时、服药第3个月、服药第6个月对患者进行随访,观察3组患者心功能、焦虑抑郁评分变化,同时观察患者不良反应的发生情况,比较心悦胶囊与艾司西酞普兰在慢性心力衰竭合并焦虑抑郁患者中的有效性及安全性。结果 3组患者治疗前后纽约心功能分级(NYHA)、左室舒张末内径、射血分数、氨基末端脑钠肽前体、收缩压差值比较,差异均无统计学意义(P>0.05)。3组患者治疗前后明尼苏达心力衰竭生活质量量表(MLHFQ)、PHQ-9健康问卷(PHQ-9)、7项广泛性焦虑障碍量表(GAD-7)评分差值比较,差异均有统计学意义(P <0.05),治疗后心悦胶囊组和艾司西酞普兰组MLHFQ评分、PHQ-9评分、GAD-7评分差值降低幅度大于常规治疗组(P <0.05),心悦胶囊组与艾司西酞普兰组治疗前后MLHFQ评分、PHQ-9评分、GAD-7评分差值比较,差异均无统计学意义(P>0.05)。3组患者治疗前后肌酐、尿素氮、丙氨酸氨基转移酶、天门冬氨酸氨基转移酶、总蛋白、钠离子、钾离子水平差值比较,差异均无统计学意义(P>0.05)。常规治疗组不良反应发生率最低、艾司西酞普兰组不良反应发生率最高(P <0.05)。结论 心悦胶囊联合常规抗心衰治疗在改善慢性心力衰竭患者心功能的同时还可进一步改善患者焦虑抑郁症状、提高生活质量,且副作用少,有很好的有效性和安全性。

艾司西酞普兰联合团体正念减压治疗与团体认知行为治疗对广泛性焦虑障碍患者的影响

目的:探讨艾司西酞普兰联合团体正念减压治疗(mindfulness based stress reduction,MBSR)及团体认知行为治疗(cognitive behavior therapy,CBT)对广泛性焦虑障碍(generalized anxiety disorder,GAD)患者的焦虑、抑郁症状的效果。方法:纳入2019年10月至2021年10月本院收治的GAD患者78例,依编号随机法分为MBSR组(43例)和CBT组(35例)。MBSR组给予口服艾司西酞普兰联合团体MBSR;CBT组给予口服艾司西酞普兰联合团体CBT。分别于基线时(T0)、8周末(T1)、干预结束3个月后(T2)用汉密尔顿焦虑量表(Hamilton anxiety scale,HAMA)、汉密尔顿抑郁量表(Hamilton depression scale,HAMD)测评2组患者的焦虑、抑郁情况,并进行分析。结果:两组共完成63例(MBSR组36例,CBT组27例)。T0时,2组患者的HAMA、HAMD评分差异无统计学意义;T1、T2时,2组HAMA、HAMD评分均显著降低(P均<0.05);2组间评分差异无统计学意义。结论:艾司西酞普兰联合团体正念减压治疗或团体认知行为治疗均能明显改善GAD患者的焦虑、抑郁水平,且持续有效。

艾司西酞普兰联合运动方案对苯二氮[艹卓]类药物依赖焦虑症患者睡眠质量的影响

目的:探讨艾司西酞普兰联合运动方案对苯二氮[艹卓]类(BDZ)药物依赖焦虑症患者睡眠质量的影响。方法:选取2021年9月至2023年2月泉州市第三医院收治的BDZ类药物依赖焦虑症患者120例作为研究对象,按照抛掷法随机分为对照组(n=58)和观察组(n=62)。对照组仅予以艾司西酞普兰治疗,观察组予以艾司西酞普兰联合运动方案治疗。比较2组睡眠质量、失眠程度、负性情绪以及生命质量。结果:治疗后,观察组匹兹堡睡眠质量指数(PSQI)中主观睡眠质量、入睡时间、睡眠效率、睡眠障碍、日间功能5个维度评分及总分均低于对照组,差异均有统计学意义(均P<0.05),失眠严重程度指数(ISI)评分低于对照组,差异有统计学意义(P<0.05);观察组汉密尔顿焦虑抑郁量表(HADS)评分均较对照组低,差异有统计学意义(P<0.05),健康调查简表(SF-36)评分较对照组高,差异有统计学意义(P<0.05)。结论:艾司西酞普兰联合运动方案能明显提高BDZ类药物依赖焦虑症患者的睡眠质量,改善失眠症状,缓解负性情绪,提高生命质量。

盐酸舍曲林和草酸艾司西酞普兰用于抑郁症治疗的安全性比较:基于FAERS数据库不良事件分析

目的通过对美国FDA不良事件报告系统(FAERS)数据库的数据挖掘,探讨盐酸舍曲林和草酸艾司西酞普兰的安全性差异。方法采用报告比值比(ROR)法和比例报告比值比(PRR)法,对FAERS数据库中2011年第1季度至2023年第2季度报告的盐酸舍曲林和草酸艾司西酞普兰的不良事件进行数据挖掘。结果女性发生不良事件的比例高于男性(男女比例约为1∶2)。盐酸舍曲林和草酸艾司西酞普兰均在18~64岁年龄组中的报告频率更高。累及系统器官分布方面,盐酸舍曲林组和草酸艾司西酞普兰组相似,但在生殖系统及乳腺疾病毒性方面存在差异,盐酸舍曲林的生殖器感觉减退信号更多,草酸艾司西酞普兰则更影响溢乳。在检测到的前10个报告信号中,药物相互作用、药物无效、恶心、头晕、头痛、焦虑的信号在盐酸舍曲林和草酸艾司西酞普兰中均有生成,盐酸舍曲林组中发生自杀意念、药物相互作用、震颤、焦虑等不良事件的可能性更大,草酸艾司西酞普兰组中更可能发生产品替换问题、妊娠期胎儿暴露、药物相互作用,提示二者的高频不良事件之间存在差异。结论盐酸舍曲林和草酸艾司西酞普兰具有相同的部分高频不良事件、相似的全身器官分布和相似的总体安全性,但在精神病类和各类检查方面存在差异,草酸艾司西酞普兰出现心电图QT间期延长不良信号强,用药后应定期复查心电图,减少晕厥、心脏骤停或死亡的风险。盐酸舍曲林出现自杀想法的信号强度高,应重视患者在治疗期间持续出现自杀想法。

补肾健脑法治疗帕金森病的疗效观察

目的探究艾司西酞普兰联合乌灵胶囊治疗帕金森病的疗效及对血清去甲肾上腺素(NE)、5-羟色胺(5-HT)、白细胞介素-1β(IL-1β)、脑源性神经营养因子(BDNF)水平的影响。方法选取2018年6月至2020年8月在济南市人民医院接受治疗的90例帕金森病患者,在组间基线特征匹配的基础上,按照随机数字表法分为联合组(45例)和对照组(45例)。其中联合组给予乌灵胶囊联合艾司西酞普兰治疗,对照组给予艾司西酞普兰治疗。对比两组患者日常生活活动能力评定量表(ADL)、帕金森统一评分量表(UPDRS)评分,血清5-HT、BDNF、NE、IL-1β水平及临床疗效。结果治疗后,两组患者血清IL-1β、UPDRS评分均降低,且联合组更低(P<0.05);ADL评分、5-HT、BDNF、NE均升高,且联合组更高(P<0.05);联合组患者的总有效率为91.11%,高于对照组的71.11%,差异有统计学意义(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)。结论乌灵胶囊联合艾司西酞普兰治疗帕金森病,可有效提高血清5-HT、BDNF、NE水平,降低血清IL-1β水平,减轻患者炎症反应,提升日常生活能力,安全有效。

艾司西酞普兰对脑梗死后抑郁症患者心理状态的影响

目的探析脑梗死后抑郁症(PCID)患者采用艾司西酞普兰治疗的临床效果。方法随机选取92例PCID患者为对象,奇偶法分为对照组和观察组,各46例。两组均接受脑梗死常规对症治疗,对照组增加氟哌噻吨美利曲辛治疗,观察组增加艾司西酞普兰治疗。比较两组神经功能、心理状态、神经递质与临床疗效。结果观察组总有效率97.83%高于对照组的80.43%(P<0.05);治疗后,观察组汉密尔顿焦虑量表(HAMA)、汉密尔顿抑郁量表(HAMD)评分(4.12±0.12)、(4.11±0.36)分较对照组的(7.36±0.65)、(7.63±1.23)分低,简易智力状态检查量表(MMSE)评分(26.25±3.15)分较对照组的(23.15±1.24)分高(P<0.05)。治疗后,观察组美国国立卫生研究院卒中量表(NIHSS)评分(4.12±0.13)分较对照组的(6.12±0.52)分低,Barthel指数(BI)评分(76.49±4.62)分较对照组的(72.25±2.36)分高(P<0.05);治疗后,观察组进食、洗澡、修饰、穿衣、控制大便、控制小便、如厕、床椅转移、平地行走、上下楼梯评分分别为(8.56±0.36)、(8.69±0.45)、(8.69±0.63)、(8.78±0.46)、(8.82±0.15)、(8.96±0.32)、(8.88±0.25)、(9.11±0.56)、(8.68±0.46)、(8.89±0.47)分,高于对照组的(7.69±0.65)、(7.71±0.33)、(7.63±0.34)、(7.89±0.34)、(7.25±0.64)、(8.12±0.11)、(7.96±0.15)、(7.86±0.13)、(7.89±0.31)、(7.86±0.36)分(P<0.05)。观察组不良反应发生率2.17%低于对照组的17.39%(P<0.05)。结论在脑梗死常规对症基础上,PCID患者治疗中使用艾司西酞普兰的效果显著,能快速改善患者神经功能,提高患者日常生活能力,缓解焦虑、抑郁症状,提高患者认知功能,具有较高的用药安全性。