Selective serotonin reuptake inhibitors and Alzheimer’s disease

Given the failure to develop disease-modifying therapies for Alzheimer’s disease(AD),strategies aiming at preventing or delaying the onset of the disease are being prioritized.While the debate regarding whether depression is an etiological risk factor or a prodrome of AD rages on,a key determining factor may be the timing of depression onset in older adults.There is increasing evidence that untreated early-onset depression is a risk factor and that late-onset depression may be a catalyst of cognitive decline.Data from animal studies have shown a beneficial impact of selective serotonin reuptake inhibitors on pathophysiological biomarkers of AD including amyloid burden,tau deposits and neurogenesis.In humans,studies focusing on subjects with a prior history of depression also showed a delay in the onset of AD in those treated with most selective serotonin reuptake inhibitors.Paroxetine,which has strong anticholinergic properties,was associated with increased mortality and mixed effects on amyloid and tau deposits in mice,as well as increased odds of developing AD in humans.Although most of the data regarding selective serotonin reuptake inhibitors is promising,findings should be interpreted cautiously because of notable methodological heterogeneity between studies.There is thus a need to conduct large scale randomized controlled trials with long follow up periods to clarify the dose-effect relationship of specific serotonergic antidepressants on AD prevention.

Relationship between use of selective serotonin reuptake inhibitors and irritable bowel syndrome: A populationbased cohort study

AIM To investigate the relationship between selective serotonin reuptake inhibitor(SSRI)use and the subsequent development of irritable bowel syndrome(IBS).METHODS This retrospective,observational,population-based cohort study collected data from Taiwan’s National Health Insurance Research Database.A total of 19653patients newly using SSRIs and 78612 patients not using SSRIs,matched by age and sex at a ratio of 1:4, were enrolled in the study from January 1,2000 to December 31,2010.The patients were followed until IBS diagnosis,withdrawal from the National Health Insurance system,or the end of 2011.We analyzed the effects of SSRIs on the risk of subsequent IBS using Cox proportional hazards regression models.RESULTS A total of 236 patients in the SSRI cohort(incidence,2.17/1000 person-years)and 478 patients in the comparison cohort(incidence,1.04/1000 person-years)received a new diagnosis of IBS.The mean follow-up period from SSRI exposure to IBS diagnosis was 2.05years.The incidence of IBS increased with advancing age.Patients with anxiety disorders had a significantly increased adjusted hazard ratio(a HR)of IBS(a HR=1.33,95%CI:1.11-1.59,P=0.002).After adjusting for sex,age,urbanization,family income,area of residence,occupation,the use of anti-psychotics and other comorbidities,the overall a HR in the SSRI cohort compared with that in the comparison cohort was1.74(95%CI:1.44-2.10;P<0.001).The cumulative incidence of IBS was higher in the SSRI cohort than in the non-SSRI cohort(log-rank test,P<0.001).CONCLUSION SSRI users show an increased risk of subsequent diagnosis of IBS in Taiwan.

Mouse strain differences in selective serotonin reuptake inhibitors sensitivity correlates with serotonin transporter binding and function

OBJECTIVE Selective serotonin reuptake inhibitors(SSRIs) bind 5-HT transporters,leading to the accumulation of 5-HT and amelioration of depression.Although different mouse strain showed different sensitivity to SSRIs in mouse models of depression,the reason for these strain differences remains unclear.Here,therefore,in the present study,we examined immobility time and locomotor activity in two mouse strains,namely,C57BL/6 J and DBA/2 J mice,and the effects of the SSRIs fluoxetine.Furthermore,we analyzed 5-HT transporter binding and reuptake inhibition in both strains to explore their relationship with the immobility and locomotor activity effects of the three SSRIs in these two mouse strains.METHODS Strain differences in SSRI effects in the tail suspension test(TST) and forced swimming test(FST).To initiate our studies,we sought to confirm that SERT strain variation did not alter SERT protein expression,5-HT recognition,or uptake activity when expressed in C57BL/6 J and DBA/2 J mice.Radioligand binding assays were conducted to determine the affinity of the SSRIs for the 5-HT transporters in the two mouse strains.RESULTS SSRI citalopram dose-dependently reduced immobility time in both the FST and TST in DBA/2 J but not C57BL/6 J mouse strains,whereas fluoxetine showed opposite results.Paroxetine reduced immobility time similarly in both strains.The affinity of citalopram for the 5-HT transporter in DBA/2 J mice was 700-fold higher than that for in C57BL/6 J mice,whereas the affinity of fluoxetine in C57BL/6 J mice was 100-fold higher than that in the DBA/2 J mouse.Furthermore,High citalopram concentrations were required to [3 H]5-HT uptake in C57BL/6 J but not DBA/2 J mouse cortical synaptosomes,whereas fluoxetine also showed opposite results.CONCLUSION Immobility duration depends on 5-HT transporter binding levels,leading to apparent strain differences in immobility time in FST and TST.Furthermore,differences in 5-HT transporter binding may cause variations in SSRI responses on behaviors.SERT mutation mice maintained sensitivity to paroxetine,an antidepressant that is unaffected by the mouse mutation.Therefore,the background strain of these mice likely contributes to the acute behavioral actions of SSRIs in immobility time.These differences may help to explain some of the discrepancies in studies that used these strains of mice to examine the role of 5-HT in mouse models of depression.Future studies should investigate additional neural substrates and molecular mechanisms underlying strain variations in mouse models of depression to help identify genetic predispositions to this disorder in humans.

Serotonin syndrome controversies:A need for consensus

Serotonin syndrome(SS)is a drug-induced clinical syndrome resulting from increased serotonergic activity in the central nervous system.Although more than seven decades have passed since the first description of SS,it is still an enigma in terms of terminology,clinical features,etiology,pathophysiology,diagnostic criteria,and therapeutic measures.The majority of SS cases have previously been reported by toxicology or psychiatry centers,particularly in people with mental illness.However,serotonergic medications are used for a variety of conditions other than mental illness.Serotonergic properties have been discovered in several new drugs,including over-the-counter medications.These days,cases are reported in non-toxicology centers,such as perioperative settings,neurology clinics,cardiology settings,gynecology settings,and pediatric clinics.Overdoses or poisonings of serotonergic agents constituted the majority of the cases observed in toxicology or psychiatry centers.Overdose or poisoning of serotonergic drugs is uncommon in other clinical settings.Patients may develop SS at therapeutic dosages.Moreover,these patients may continue to use serotonergic medications even if they develop mild to moderate SS due to several reasons.Thus,the clinical presentation(onset,severity,and clinical features)in such instances may not exactly match what toxicologists or psychiatrists observe in their respective settings.They produce considerable diversity in many aspects of SS.However,other experts discount these new developments in SS.Since SS is a potentially lethal illness,consensus is required on several concerns related to SS.

Fluoxetine,a selective serotonin reuptake inhibitor used clinically,improves bladder function in a mouse model of moderate spinal cord injury

After spinal cord injury,the upward conduction of the spinal cord is lost,resulting in the loss of micturition control,which manifests as detrusor sphincter dyssynergia and insufficient micturition.Studies have shown that serotonergic axons play important roles in the control of the descending urination tract.In this study,mouse models of moderate spinal cord contusions were established.The serotonin agonists quipazine(0.2 mg/kg),8-hydroxy-2-(di-n-propylamino)tetralin(8-OH-DAPT,0.1 mg/kg),buspirone(1 mg/kg),sumatriptan(1 mg/kg),and rizatriptan(50 mg/kg),the serotonin reuptake inhibitors fluoxetine(20 mg/kg)and duloxetine(1 mg/kg),and the dopamine receptor agonist SKF-82197(0.1 mg/kg)were intraperitoneally administered to the model mice 35 days post-injury in an acute manner.The voided stain on paper method and urodynamics revealed that fluoxetine reduced the amount of residual urine in the bladder and decreased bladder and external urethral sphincter pressure in a mouse model of moderate spinal cord injury.However,fluoxetine did not improve the micturition function in a mouse model of severe spinal cord injury.In contrast,the other serotonergic drugs had no effects on the micturition functions of spinal cord injury model mice.This study was ethically approved by the Institutional Animal Care and Use Committee of Jiangsu Province Hospital of Chinese Medicine(approval No.2020DW-20-02)on September 11,2020.

基于美国FAERS数据库抗抑郁药物与胎儿及新生儿的不良事件信号分析

目的基于美国食品药品监督管理局不良事件报告系统(FAERS)挖掘抗抑郁药物的使用与胎儿及新生儿不良事件的风险信号,为临床安全合理用药提供参考。方法筛选FAERS数据库2004年1月1日至2022年12月31日中怀疑抗抑郁药的不良事件报告,并通过报告比值比(ROR)法和比例报告比值比(PRR)法挖掘抗抑郁药与胎儿及新生儿之间的不良事件信号。结果共有14492例儿胎儿及新生儿异常的病例纳入研究,其中胎儿组5546例,新生儿组病例8946例。药物方面,分别有68.97%、56.35%的胎儿不良事件信号和新生儿不良事件信号为选择性5-羟色胺再摄取抑制剂(SSRI)类抗抑郁药产生。不良事件方面,51.72%胎儿不良事件信号与羊水相关,20.99%的新生儿不良事件信号与呼吸系统异常相关。对产生的不良事件信号进行二次筛选后,西酞普兰和文拉法辛信号突出,且存在说明书未载明信号。结论抗抑郁药物的整体信号特征与现有的安全性资料基本一致,但通过分组分析仍然发现了如胎儿羊水异常、新生儿心脏方面等说明书未载明不良事件,临床使用时应重点关注。

快速色氨酸耗竭试验对SSRIs药物治疗后抑郁症患者的心境和睡眠脑电图影响的系统评价和Meta分析

目的通过系统评价和Meta分析方法对比不同研究中快速色氨酸耗竭(TD)试验对经选择性5-羟色胺(5-HT)再摄取抑制剂(SSRIs)药物治疗后抑郁症患者的心境和睡眠脑电图的影响,以研究TD试验在该类抑郁症患者中作用的有效性。方法计算机检索PubMed、Cochrane图书馆、Web of Science、Embase、CBM、CNKI等相关国内外数据库,全面搜集将TD试验用于经SSRIs药物治疗后抑郁症患者研究的所有临床随机对照研究(RCT),按照Jadad标准对纳入文献进行质量分析,并使用RevMan4.2软件进行Meta分析,对不能合并的数据结果进行系统评价。结果最终纳入2篇高质量RCT研究,Jadad评分均在3分以上。系统评价结果显示,TD组研究对象体内色氨酸浓度明显降低,达到了色氨酸耗竭的标准。Meta分析结果显示,TD组患者在汉密尔顿焦虑量表-19(HRSA-19)评分[WMD 1.37、95%CI(0.76,1.99)、P<0.001]、心境量表(POMS)中的迷惑评分[WMD1.179、5%CI(0.44,1.91)、P=0.002]、睡眠相关分析中的TST值[WMD 127、95%CI(1.5,23.9)、P=0.03]、SL值[WMD-8.11、95%CI(-12.24,-3.98)、P=0.01]、RD值[WMD 0.17、95%CI(0.04,0.31)、P=0.01]以及S1值[WMD 2.52、95%CI(-0.02,5.07)、P=0.05]与对照组比较差异有统计学意义(P<0.05)。结论本研究结果证明TD试验能够诱导经SSRIs药物治疗后的抑郁症患者出现抑郁情绪及迷惑情绪,同时能影响该类患者的睡眠周期相关参数,包括缩短快动眼潜时、增加快动眼期比例、增加快动眼期内动眼频率等。而对于其他检测指标,目前尚没有足够的证据能够证明其组间差异性。受纳入研究质量限制,上述结果还有待开展更多高质量的临床RCT试验来进一步证实。

阿戈美拉汀与SSRIs治疗抑郁障碍疗效的Meta分析

目的比较阿戈美拉汀与选择性五羟色胺(5-HT)再摄取抑制剂(SSRIs)治疗抑郁障碍的疗效,为临床治疗提供循证医学参考。方法通过Medline、Pub Med、Wiley online library数据库检索英文文献,采用汉密尔顿抑郁量表(HAMD)及汉密尔顿焦虑量表(HAMA)评分减分作为抑郁症状及焦虑症状的改善指标,采用Rev Man 5.2统计软件进行Meta分析,比较阿戈美拉汀与SSRIs的疗效。结果最终纳入符合标准的文献6篇。阿戈美拉汀与SSRIs治疗抑郁症状[SMD=0.06(95%CI:-0.03,0.14)]与焦虑症状的改善效果[MD=0.12(95%CI:-0.82,1.06)]均无显著差异(P>0.05)。结论阿戈美拉汀与SSRIs治疗抑郁障碍的疗效相当。

浙江省精神专科医院抗抑郁药临床综合评价与遴选专家共识

目的引导和推动浙江省精神专科医院规范开展抗抑郁药的临床综合评价与遴选工作。方法浙江大学医学院附属精神卫生中心联合杭州市药事管理质量控制中心及浙江省内7家精神专科医院,广泛征求临床专家和药学专家的意见与建议,撰写了《浙江省精神专科医院抗抑郁药临床综合评价与遴选专家共识》,并以13种5-羟色胺再摄取抑制剂(SSRI)和5-羟色胺去甲肾上腺素再摄取抑制剂(SNRI)为例进行试点评价。结果该共识从药学特性、安全性、有效性、经济性、创新性和其他属性6个维度对纳入的抗抑郁药进行了系统评价,并在每个维度下进行二级赋分。结论该共识的制订为抗抑郁药的快速临床综合评价与遴选提供了参考依据,同时引导和推动了相关医疗机构规范开展抗抑郁药的临床综合评价与遴选工作,以满足多元化的临床用药需求,促进临床合理用药。

5-羟色胺选择性重摄取抑制剂联合计算机化的认知训练治疗伴有认知障碍的老年抑郁症患者的研究

目的探讨5-羟色胺选择性重摄取抑制剂(SSRI)联合计算机化的认知训练(CCT)对伴有认知障碍的老年抑郁症(LLD)患者的临床治疗效果。方法本研究为前瞻性随机对照临床研究。选取2021年5月至2022年12月于首都医科大学附属北京安定医院门诊及住院治疗的118例伴有认知障碍的LLD患者,按照随机数表法分为干预组(57例)和对照组(61例)。干预组给予临床常规SSRI类抗抑郁药治疗联合CCT干预,对照组给予临床常规SSRI类抗抑郁药治疗联合空白对照方法,两组均治疗12周。分别在治疗前及治疗后8、12周对两组患者进行阿尔茨海默病认知评估量表(ADAS-cog)、老年抑郁量表(GDS)及日常生活能力量表(ADL)评分,以评估其认知功能、精神心理状况及社会功能。结果在治疗后8周及12周时,两组的ADAS-cog、GDS量表评分均明显低于治疗前,且干预组明显低于对照组,差异均有统计学意义(P<0.05)。治疗后8周及12周时,干预组的ADL评分明显高于治疗前,且治疗后12周干预组的ADL评分明显高于对照组,差异均有统计学意义(P<0.05),而对照组治疗前后的ADL评分比较差异无统计学意义(P>0.05)。结论SSRI类抗抑郁药联合CCT治疗能够显著改善伴有认知障碍的LLD患者的认知功能和抑郁症状,可作为该类人群的有效选择。

盐酸文拉法辛缓释胶囊致低钠血症1例分析

目的探讨文拉法辛导致低钠血症的不良反应及影响因素,为临床安全用药提供参考。方法通过对1例使用盐酸文拉法辛缓释胶囊导致低钠血症病例进行分析,检索同类文献发表情况,并提出用药建议。结果患者长期使用文拉法辛治疗前庭性偏头痛5年后反复出现低钠血症,停用文拉法辛和对应补钠治疗后血钠逐渐恢复至正常,考虑为文拉法辛引起低钠血症。结论文拉法辛是临床上用于抑郁症治疗的主要药物之一,医生应关注文拉法辛引起低钠血症的风险,熟悉该药的适应证、禁忌证、药物相互作用和疗程,特别是高龄、女性、使用利尿剂等药物和既往有低钠血症病史的患者,用药期间定期监测电解质,从小剂量开始给药,尽早发现药品不良反应,确保患者用药安全。

Possible association of the 5-HTTLPR serotonin transporter promoter gene polymorphism with premature ejaculation in a Turkish population

We evaluated the genotypes of the serotonin transporter gene （5-HTT） in patients with premature ejaculation （PE） to determine the role of genetic factors in the etiopathogenesis of PE and possibly to identify the patient subgroups. A total of 70 PE patients and 70 controls were included in this study. All men were heterosexual, had no other disorders and were either married or in a stable relationship. PE was defined as ejaculation that occurred within 1 min of vaginal intromission. Genomic DNA from patients and controls was analyzed using polymerase chain reaction, and allelic variations of the promoter region of the serotonin transporter gene （5-HTTLPR） were determined. The 5-HTTLPR （serotonin transporter promoter gene） genotypes in PE patients vs. controls were distributed as follows： L/L 16% vs. 17%, L/S 30% vs. 53% and S/S 54% vs. 28%. We examined the haplotype analysis for three polymorphisms of the 5-HTTLPR gene： LL, LS and SS. The appropriateness of the allele frequencies in the 5-HTTLPR gene was analyzed by the Hardy-Weinberg equilibrium using the Z-test. The short （S） allele of the 5-HTTLPR gene was significantly more frequent in PE patients than in controls （P 〈 0.05）. We suggest that the 5-HTTLPR gene plays a role in the pathophysiology of all primary PE cases. Further studies are needed to evaluate the relationship between 5-HTTLPR gene polymorphism and patient subgroup （such as primary and secondary PE） responses to selective serotonin reuptake inhibitors as well as ethnic differences.

5-羟色胺1A/2A受体基因多态性与SSRIs抗抑郁疗效的相关性研究

目的:研究患者5-羟色胺1A/2A(5-HTR1A/2A)基因多态性与选择性5-羟色胺再摄取抑制剂(SSRI)类药物(SSRIs)抗抑郁疗效的相关性,为SSRIs的合理使用提供参考。方法:采用前瞻性研究方法,选取2016年10月-2017年10月内蒙古自治区人民医院精神专科符合入组标准的85例抑郁症住院患者,随机口服SSRIs帕罗西汀或舍曲林或艾司西酞普兰中的任意一种进行治疗,治疗周期为8周。以汉密尔顿焦虑量表(HAMD)评分计算所得患者治疗后的HAMD减分率为标准,分为有效组(HAMD减分率≥50%)和无效组(HAMD减分率<50%)。采用χ2检验分析两组患者5-HTR1A(rs6295)、5-HTR2A(rs6313、rs6311)的基因型分布和基因分布频率的差异,t检验比较有显著影响基因型对HAMD减分率的影响。结果:有效组患者45例,无效组患者40例,两组患者间民族、性别、年龄差异均无统计学意义(P>0.05)。两组患者5-HTR1A(rs6295)等位基因G、C的分布频率差异有统计学意义(χ2=13.75,P<0.001),基因型分布差异无统计学意义(χ2=4.72,P=0.09);5-HTR2A(rs6313)等位基因G、A和5-HTR2A(rs6311)等位基因C、T的分布频率差异均有统计学意义(χ2=15.20、15.20,P<0.001),基因型分布差异也均有统计学意义(χ2=23.68、23.68,P<0.001)。5-HTR2A(rs6313)G/A、G/G、A/A 3种基因型患者间HAMD减分率差异无统计学意义(P>0.05)。5-HTR2A(rs6311)T/T与C/C、T/T与C/T基因型患者间HAMD减分率差异无统计学意义(P>0.05),仅C/C基因型患者HAMD减分率明显高于C/T基因型患者(P=0.02)。结论:5-HTR2A(rs6313、rs6311)基因多态性可能与SSRIs治疗抑郁症的临床疗效有关,其中5-HTR2A(rs6311)C/C基因型有希望作为SSRIs治疗抑郁症时判别疗效的预测因子。

典型SSRIs类抗抑郁药对鱼类的毒性效应研究进展

选择性血清素再摄取抑制剂(selective serotonin reuptake inhibitors,SSRIs)是一类在临床上具有良好治疗效果的抗抑郁药物,由于使用量巨大,在水环境中频繁被检出,其潜在生态毒性效应引起人们的广泛关注。鱼类作为水生脊椎动物,具有和人类相似的神经调控系统,更易受到水体中残留的SSRIs的影响。本文综述了SSRIs在鱼类体内的代谢和生物积累效应,以及SSRIs对鱼类产生的生长发育毒性、生殖毒性和神经行为毒性,并对未来该领域的研究进行了展望。

Differences of Plasma Levels of Tryptophan, Serotonin, 5-Hydroxyindole Acetic Acid, and Kynurenine between Healthy People and Patients of Major Monopolar Depression at Various Age and Gender

Background: It is not well analyzed whether there are differences in plasma levels of tryptophan (TRP) metabolites between healthy control people (HC) and patients of major monopolar depression (MMD). Methods: Ultra high-speed liquid chromatography/mass spectrometry has been used for the simultaneous determination of plasma levels of tryptophan metabolites in depressive patients. Results: There are no significant differences between plasma levels of TRP between HC and MMD. Plasma levels of TRP of HC are higher in young men, young women, old men, and old women in this order. Serotonin (5-HT) levels are higher in MMD than HC. Plasma levels of 5-HIAA of HC are also higher than those of patients of MMD. Plasma levels of kynurenine (KYN) of healthy old men and old women are higher than those of young men and old women. Plasma levels of KYN are higher in old women and young men of MMD than those of HC. Conclusion: Plasma levels of 5-HT are higher in patients of MMD than those of HC, which may suggest that use of drugs inhibiting the 5-HT transportation may increase plasma levels of 5-HT in MMD.

SSRIs类药物与自杀的关系:系统综述的方法学质量评价和研究结果归纳(英文)

背景:关于使用选择性5-羟色胺再摄取抑制剂(SSRIs)与自杀意念或行为的关系,一些系统综述已发表,但是对这些报告的质量并没有做过正式的评估。目的:评估有关使用SSRI与自杀意念和行为之间关系的系统综述的方法学质量;并提供在此评估的基础上得出的总体结论。方法 :通过检索Pubmed,Embase,Cochrane图书馆,EBSCO,PsycINFO,中国国家知网,中国科技期刊重庆维普数据库,万方数据库,和中国生物医学文献数据库来确定相关的系统综述,这些系统综述纳入了比较SSRI类药物与安慰剂、以自杀意念或行为作为关键变量的随机对照试验。两个专家评估者独自采用多系统综述11项评估量表(AMSTAR)对纳入评估的文献进行方法学质量的评估。结果 :共检出12篇系统综述和meta分析。AMSTAR总体质量评分的评分者信度非常好(ICC=0.86),但11个AMSTAR项目中有5项的评分者信度较差(Kappa值<0.60)。根据AMSTAR总分,仅1篇为高质量等级,8篇为中等质量等级,3篇为低质量等级。这篇高质量综述和3篇中等质量的综述均报告SSRI组中自杀意念或行为的风险显著高于安慰剂组。4篇仅限于儿童和青少年的综述中有3篇报道服用帕罗西汀和患有抑郁症的青少年有显著增加自杀意念或行为的风险。结论 :现有证据表明,青少年使用SSRI类药物可能会增加自杀意念和行为的风险,尤其是抑郁症患者和服用帕罗西汀的患者。但是,相关高质量的综述很少,所以对这一结论还存有疑问。AMSTAR量表对于提高系统综述质量也许是有用的,但对量表中的某些项目需要严格操作标准。

SSRIs和丁螺环酮对首发强迫障碍患者疗效和认知功能的影响

目的探讨SSRIs联用丁螺环酮对首发强迫障碍患者疗效及认知功能的影响。方法将60例首发强迫障碍(OCD)患者随机分成两组,研究组接受SSRIs和丁螺环酮治疗,对照组单用SSRIs治疗,治疗时间6个月。采用YaleBrown强迫量表(Y-BOCS)、中国修订版韦氏记忆测验(WMS-RC)、Stroop色词测验(SCWT)、连线测验(TMT)A和B、威斯康星卡片分类测验(WCST)评定疗效和认知功能。结果治疗后研究组Y-BOCS总分、强迫行为因子分低于对照组(P<0.05)。治疗后研究组WMS-RC的记忆商、瞬时记忆、短时记忆评分高于对照组(P<0.05),TMT时间少于对照组(P<0.05),研究组SCWT用时低于对照组(P<0.05)。治疗后研究组WCST错误应答数、持续错误数均少于对照组(P<0.05)。研究组治疗后的Y-BOCS总分、强迫观念因子分、强迫行为因子分均低于治疗前(P<0.05),WMS-RC的记忆商、瞬时记忆、短时记忆分均高于治疗前(P<0.05),TMT时间少于治疗前(P<0.05),SCWT的错误数及用时均低于治疗前(P<0.05),WCST的正确应答数多于治疗前,错误应答数、持续错误数均显著少于治疗前(P<0.05)。结论 SSRIs联合丁螺环酮可有效改善强迫障碍患者的临床症状和认知功能。

疏肝益肾起痿汤联合他达拉非片治疗5-羟色胺再摄取抑制剂类抗抑郁药所致勃起功能障碍临床研究

目的:观察疏肝益肾起痿汤联合他达拉非片治疗5-羟色胺再摄取抑制剂(SSRIs)类抗抑郁药所致勃起功能障碍(ED)患者的效果。方法:选取112例肝郁肾虚型SSRIs类抗抑郁药所致ED患者,采用随机数字表法分为2组各56例,对照组给予他达拉非片治疗,观察组给予疏肝益肾起痿汤联合他达拉非片治疗,2组均治疗8周。对比2组临床疗效,治疗前后评定中医证候评分、勃起功能[勃起硬度评价量表(EHS)评分、国际勃起功能评分量表(IIEF-5)评分]、心理状态[抑郁症筛查量表(PHQ-9)评分]、血管内皮功能[血清内皮素-1(ET-1)、一氧化氮(NO),血管扩张功能(FMD)],观察治疗期间的不良反应。结果:治疗后,观察组临床疗效优于对照组(P<0.05)。2组性欲下降、阴茎痿软不举、阴茎举而不坚、忧愁善感、小便淋漓评分及PHQ-9评分均较治疗前降低(P<0.05),观察组6项评分均低于对照组(P<0.05)。2组EHS评分、IIEF-5评分均较治疗前升高(P<0.05),观察组EHS评分、IIEF-5评分均高于对照组(P<0.05)。2组ET-1水平均较治疗前降低,NO水平及FMD值均较治疗前升高,差异均有统计学意义(P<0.05)。观察组ET-1水平低于对照组,NO水平及FMD值均高于对照组,差异均有统计学意义(P<0.05)。2组患者均未发生明显不良反应。结论:采用疏肝益肾起痿汤联合他达拉非片治疗肝郁肾虚型SSRIs类抗抑郁药所致ED效果明显,能够改善患者的心理状态和血管内皮功能,提高勃起功能,安全性高。

乌鸡白凤丸对选择性5-羟色胺再摄取抑制剂引起的性功能障碍的效果分析

目的 观察乌鸡白凤丸对选择性5-羟色胺再摄取抑制剂(selective serotonin reuptake inhibitors,SSRIs)引起的性功能障碍的临床效果。方法 收集2017年6月1日-2021年6月1日在本院就诊的60例因抑郁症服用SSIRs而导致性功能障碍的患者为研究对象,按照随机数字表法将其分为对照组和观察组,每组各30例。对照组予继续以原基础治疗药物,观察组则在对照组基础上联合乌鸡白凤丸口服。对比观察两组患者在治疗前、治疗2周、治疗4周、治疗8周(治疗结束)的抑郁评分量表评分、性功能障碍评分量表评分的差异,并观察治疗不良反应及患者的满意度。结果 治疗前,两组患者的HAMD、ASEX评分对比无明显差异(P>0.05),随着治疗的进行,对照组患者的HAMD及ASEX评分无明显变化(P>0.05),而观察组患者的HAMD及ASEX评分均明显降低(P<0.05),在治疗的同时期(治疗2周、4周及8周),观察组患者的HAMD评分及ASEX评分均显著低于对照组(P<0.05)。治疗前,两组患者在肝肾功能、甲状腺功能、血脂及血糖相关化验指标上无明显差异(P<0.05),治疗后,对照组患者的各项化验指标仍无明显改变(P>0.05),而观察组患者TG水平较治疗前明显升高(P<0.05),同时治疗后观察组患者TG水平较对照组明显升高(P<0.05)。观察组患者对治疗的满意度高于对照组(P<0.05)。结论 乌鸡白凤丸治疗SSRIs引起的性功能障碍具有良好的效果及安全性。

虚汗停颗粒联合5-羟色胺选择性重摄取抑制剂治疗抑郁症临床观察

目的:通过虚汗停颗粒联合5-羟色胺选择性重摄取抑制剂(SSRI)与单用SSRI比较,探究其安全性及对抑郁症患者健康相关生命质量的影响。方法:选取2017年1月至2019年12月中山大学附属第三医院收治的抑郁障碍急性发作患者95例作为研究对象,采用随机数字表法将患者分为观察组(n=46)和对照组(n=49)。对照组单用SSRI,观察组在对照组基础上联合口服虚汗停颗粒,2组均治疗8周。期间定期访视并测定抑郁自评量表(SDS)评分、健康调查量表36(SF-36)评分、哥伦比亚-自杀严重性评定量表(C-SSRS)评分、Barnes静坐不能量表(BAS)评分及异常不自主运动量表(AIMS)评分。结果:治疗8周后,与对照组比较,观察组患者SDS评分显著降低(P<0.01),而SF-36评分无显著性差异。在安全性方面,与对照组比较,观察组C-SSRS评分无显著性差异,而BAS及AIMS评分则显著降低(P<0.01)。结论:虚汗停颗粒联合SSRI类抗抑郁药治疗抑郁症患者,可以有效改善患者的社会功能,减少锥体外系不良反应,且安全性较高。