Modulation of the suppressive effect of corticosterone on adult rat hippocampal cell proliferation by paroxetine

Objective The literature has shown that cognitive and emotional changes may occur after chronic treatment with glucocorticoids. This might be caused by the suppressive effect of glucocorticoids on hippocampal neurogenesis and cell proliferation. Paroxetine, a selective serotonin reuptake transporter, is a commonly used antidepressant for alleviation of signs and symptoms of clinical depression. It was discovered to promote hippocampal neurogenesis in the past few years and we wanted to investigate its interaction with glucocorticoid in this study. Methods Adult rats were given vehicle, corticosterone, paroxetine, or both corticosterone and paroxetine for 14 d. Cell proliferation in the dentate gyrus was quantified using 5-bromo-2-deoxyuridine （BrdU） immunohistochemistry. Results The corticosterone treatment suppressed while paroxetine treatment increased hippocampal cell proliferation. More importantly, paroxetine treatment could reverse the suppressive effect of corticosterone on hippocampal cell proliferation. Conclusion This may have clinic application in preventing hippocampal damage after glucocorticoid treatment.

Comparison of paroxetine and dapoxetine, a novel selective serotonin reuptake inhibitor in the treatment of premature ejaculation

Dapoxetine hydrochloride is a selective serotonin reuptake inhibitor and the first drug approved for the on-demand treatment of premature ejaculation （PE）, Our objective in this study was to characterize the efficacy of on-demand dapoxetine （30 and 60 mg） and daily paroxetine （20 mg） usage in treating PE, We conducted a 1 month study involving a total of 150 patients. Patients were divided into three groups of 50, Group 1 were treated with on-demand dapoxetine （30 mg）, Group 2 with on-demand dapoxetine （60 mg） and Group 3 with daily paroxetine （20 rag）, Our outcome measurement was increased from baseline intravaginal ejaculatory latency time （IELT） after treatment, The IELT increased from baseline to posttreatment by 117%, 117% and 170% in the paroxetine group （P 〈 0,01）, 30 mg dapoxetine group （P 〈 0,01） and 60 mg dapoxetine group （P 〈 0.01）, respectively, The increase from baseline IELT were similar for the 30 mg dapoxetine and paroxetine groups （P 〉 0,05）, while the 60 mg dapoxetine group had a larger posttreatment IELT increase compared with the 30 mg dapoxetine （P〈 0.05） and paroxetine （P〈 0.01） groups, Dapoxetine （60 mg） 1-3 h before planned intercourse is a very effective treatment modality for PE. However, an on-demand dose of 30 mg dapoxetine is no more effective than the currently prescribed paroxetine treatment.

Improvement in quality of life in depressed patients following verum acupuncture or electroacupuncture plus paroxetine:A randomized controlled study of 157 cases

Depressed patients with scores of 17 or more on the 17 items of the Hamilton Depression Rating Scale were treated with the antidepressant drug paroxetine. They also underwent verum acupuncture or electroacupuncture at Baihui （GV20） and Yintang （GV29）. The World Health Organization Quality of Life Scale Brief Version showed a significant increase in the total scores of patients who underwent verum acupuncture and electroacupuncture for 6 weeks compared with those who were given paroxetine only; significantly increased physical domain and social relationship scores in verum acupuncture patients compared with paroxetine only; and significantly elevated psychological domain scores with electroacupuncture compared with paroxetine only. These results indicate that both verum acupuncture and electroacupuncture can improve quality of life in depressed patients undergoing paroxetine treatment,

Paroxetine engenders analgesic effects through inhibition of p38 phosphorylation in a rat migraine model

In this study, a model of migraine was established by electrical stimulation of the superior sagittal sinus in rats. These rats were then treated orally with paroxetine at doses of 2.5, 5, or 10 mg/kg per day for 14 days. Following treatment, mechanical withdrawal thresholds were significantly higher, extracellular concentrations of 5-hydroxytryptamine in the periaqueductal grey matter and nucleus reticularis gigantocellularis were higher, and the expression of phosphorylated p38 in the trigeminal nucleus caudalis was lower. Our experimental findings suggest that paroxetine has analgesic effects in a rat migraine model, which are mediated by inhibition of p38 phosphorylation.

Paroxetine vs pregabalin for the management of neuropathic pain in multiple sclerosis

AIM: To compare the effectiveness and tolerability of paroxetine vs pregabalin for the management of multiple sclerosis(MS)-induced neuropathic pain(NPP).METHODS: A randomized, flexible-dose open-label 8-wk study involving 21 relapsing-remitting MS patients with MS-induced NPP was conducted to evaluate the effectiveness and tolerability of pregabalin versus paroxetine for pain management. The trial included a 3-wk dose titration phase followed by a 5-wk stable dose phase. Primary outcome measures included daily patient-reported pain intensity as measured using a 100 mm visual analogue scale(VAS pain) and daily impact of pain on daily activities(VAS impact). Hierarchical regression modeling was conducted on each outcome to determine if within person VAS trajectory for pain and impact differed across study groups, during 56 d follow-up. RESULTS: Attrition rates were significantly greater(P < 0.001) in the paroxetine versus pregabalin study group(70% vs 18.2%, respectively). Average study duration between study groups also significantly differed(P < 0.001). Paroxetine participants completed an average of 27.3 d of treatment vs 49.5 d in the pregabalin group, with the majority of patients withdrawing due to adverse events. Due to the high attrition rates in the paroxetine study arm, the investigators stopped the study prior to achieving complete recruitment. As such, no significant differences between pregabalin and paroxetine study arms were noted for the primary outcome measures(VAS pain, VAS impact). Comparative assessment of baseline patient characteristics also revealed no significant differences between the study arms. CONCLUSION: High attrition rates associated with paroxetine use suggest that it be used with caution for MS-induced NPP. Efficacy outcomes could not be assessed due to attrition.

The Effect of Paroxetine on Depressive Symptom with Somatic Disease and Change of Platelet 5-HT Concentration

To study the effect of paroxetine on depressive symptom accompanying somatic disease and the value of platelet 5-HT concentration in the diagnosis of depression, 30 patients with depressive symptom were treated with paroxetine. All patients were evaluated on Zung and HAMD scale and assayed of platelet 5-HT concentration before and after treatment. It was found that patients had a lower level of platelet 5-HT concentration than healthy people (P<0.01). After six weeks of treatment, depressive and somatic symptoms were both improved (P<0.01) and platelet 5-HT concentration was even lower (P>0.05). It was suggested that paroxetine was a good antidepressant and platelet 5-HT concentration was useful in the screening of depression.

Administration of Zinc with Paroxetine Improved the Forced Swim Test Behavioral Pattern of Treated Mice in Acute and Sub-Acute Study

Despite progressive improvement in treating major depressive disorder (MDD), it remains mostly unresponsive to one antidepressant medication. Zinc is a brain highly abundant trace metal, a brain derived neurotrophic factor (BDNF) inducer, a modulator of synaptic plasticity and potent suppressor of the NMDA receptors. We proposed that co-administration of zinc with the antide-pressants may represent a valuable regimen to improve the efficacy of these drugs. This work has been implemented to evaluate the behavioral changes of acute and sub-acute co-administration of zinc with Paroxtine in mice. Methods: The animals were injected intra-peritoneal with either Paroxtine (20 mg/kg) which was a selective serotonin reuptake inhibitor (SSRI), zinc sulfate (30 mg/kg) or Paroxtine in combination with zinc for one day and one week (once daily). The pattern of the animal behavior was assessed in the forced swim test (FST). Results and Discussion: The behavioral patterns of the animals in the FST include immobility, swimming and climbing. Successful antidepressant should decrease the immobility time with either increase in swimming and/or climbing behavior based on the drug pharmacological activity. Our results revealed a significant decrease of immobility and increase of swimming behavior indicating serotonin-dependent pharmacological activity of Paroxtine or zinc alone as well as in the animals treated with zinc in combination with Paroxtine. There was no significant difference in the animals’ behavior between acute and sub-acute treatment with zinc or even upon its addition to paroxetine. Our data support the concept that co-administration of zinc may provide further antidepressant activity. Zinc may offer additional clinical value particularly in geriatric patients or other populations where zinc level has shown dramatic decrease.

Rate of social anxiety disorder, its comorbidity with depression and paroxetine effects in outpatients in Japan

The prevalence of persons with social anxiety disorder (SAD) in Japan remains unknown. This study examined 293 patients with age between 20 and 60 at first visit on the outpatient clinic of psychiatry by the section of social phobia of M.I.N.I. and DSM-IV. After that, 10 patients with both SAD out of 16 patients (trial recruited) completed 12 weeks of treatment with paroxetine. Among 63 patients with 4 points and 40 patients with 3 points on the M.I.N.I., 21 patients (33%) and 16 patients (40%) were diagnosed as SAD on DSM-IV criteria, respectively. Together, 37 patients (12.6%) were diagnosed as SAD out of the 293 outpatients. Among 37 patients with SAD, 23 patients (62%) had comorbid depression. As for 10 patients after treatment with paroxetine, 8 patients improved from the point of recovery of depression (HAM-D scores below 10), whereas only 4 patients improved from the point of recovery of social phobia (L-SAS scores below 30). Three points as well as 4 points on the M.I.N.I. is meaningful for the diagnosis of SAD. For a while, paroxetine exerted less beneficial effects on SAD rather than on depression.

Influence of paroxetine and cognitive/behavioral strategies in neurocardiogenic syncope and depression: a case report

OBJECTIVE: Neurocardiogenic syncope (NCS) is a condition where the patient has a temporary loss of consciousness or feelings of weakness and fatigue. There are triggers such as prolonged sitting or standing, pain, and heavy exercise, but often episodes are random. Treatments are limited and the use of specific serotonin reuptake inhibitors (SSRI) have had mixed results, but a limited number of studies have suggested that paroxetine may be effective in improving the symptoms of NCS. METHODS: This is a single case report of a 20-year old female who was diagnosed with NCS by a tilt test and treated conservatively with increased fluid and salt intake, and counter-pressure maneuvers. She was given one dose of sertraline, but immediately experienced disturbing visual images. She presented at the Depression Center with moderate depressive symptoms and was started on paroxetine and given cognitive/behavioral strategies to manage the NCS. RESULTS: Since the patient had a negative experience with a prior SSRI, she was started on a low dose of paroxetine and omega-3 fatty acids. She also was given a detailed explanation of NCS and a number of cognitive/behavioral strategies such as deep breathing, progressive relaxation, imagery, and sleep. CONCLUSION: After 2-weeks of the multi-faceted treatment approach, she had a significant decrease in her depressive symptoms. After 6-months, the patient had no episodes of syncope and no depressive symptoms. She was able to stand for long periods and exercise without feelings of weakness and fatigue. A multimodal approach may offer the best treatment strategy to achieve full remission in patients with NCS.

Paroxetine Augments while Naloxone Abolishes the Analgesic Effect of Paracetamol in Acute Nociceptive Pain in Mice

The mechanism(s) of analgesic action of paracetamol (acetaminophen;N-acetyl-p-aminophenol) remains controversial. Previous studies on rats suggested that the antinociceptive action of paracetamol might involve the central descending inhibitory pain pathways recruiting both a serotoninergic and an opioidergic system. This study explores this issue in mice using paroxetine, the most potent selective serotonin re-uptake inhibitor, and the nonselective opioid pure antagonist naloxone. Animals were divided into two main groups for two separate experiments, each subdivided into 3 subgroups. In both experiments;the first group served as control, the second group received paracetamol (200 mg/kg, i.p). In one experiment, the third group received paroxetine (20 mg/kg p.o for 7 days) before paracetamol. In the other experiment, animals of the third group were pretreated with naloxone (5 mg/kg, i.p) 30 min before paracetamol. The antinociceptive effect of paracetamol was tested using the hot plate test. Paracetamol displayed a significant antinociceptive activity that was augmented by pretreatment with paroxetine as was shown by maintenance of its effect beyond that shown by paracetamol alone. On the other hand, pretreatment with naloxone abolished paracetamol’s antinociceptive activity in the hot-plate test. These results extended the previous observation in rats that the antinociceptive effect of paracetamol involved activation of a central descending pain inhibitory pathway with serotonin and opioidergic peptides being potential mediators recruited.

THE EFFECTS OF ELECTRO-ACUPUNCTURE VS. AMITRIPTYLINE ON PLATELET 3H-PAROXETINE BINDING SITES IN DEPRESSED PATIENTS

In this study platelet 3H-paroxetine binding site was studied in 16 depressed pa-tients and 16 healthy volunteers. We found that the mean Bmax of 3H-paroxetine binding on theplatelets of depressed patients was significantly lower than that of normal controls. After treated withamitriptyline or electro-acupuncture for 6 weeks, the density of paroxetine binding sites increased to-wards normal in well responded patients. But no significant difference was found between electro-acupuncture and amitriptyline as compared in their effects on 3H-paroxetine binding sites.

Effects of paroxetine on function recovery in patients with poststroke depression

Objective To evaluate the effects of the selective serotonin reuptake inhibitor(SSRI) paroxetine on the functional capacities of poststroke depression.Method Seventy five patients were randomly assigned to 3 groups,during 8 weeks of therapy,patients were treated wtih paroxetine,doxepin, and placebo.Before and at the end of the observation,we assessed ADL by Barthel index,degree of neurological deficit by Chinese stroke scale and depressive symptomatology by Hamilton depression rating scale.Results The three groups ameliorated ADL capacities and neurological deficitto different extents.The greatest improvement was observed in the paroxetine treated group.Conclusion Paroxetine may facilitate recovery in patients with poststroke depression undergoing rehabilitation.The effects of SSRI as an adunct to physical therapy warrant further investigation.

帕罗西汀联合共情技术对不同年龄高血压合并焦虑抑郁患者身心的影响

目的观察帕罗西汀联合共情技术对不同年龄高血压合并焦虑抑郁患者身心状态的影响。方法选取高血压合并焦虑抑郁患者120例,根据年龄分为中青年组与老年组,每组60例。2组均采用帕罗西汀联合共情技术干预,比较2组治疗依从性、干预前后血压[收缩压(special boiling point,SBP)、舒张压(diastolic blood pressure,DBP)]、汉密尔顿焦虑量表(Hamilton anxiety scale,HAMA)评分、汉密顿抑郁量表(Hamilton depression scale,HAMD)评分、共情能力、生活质量和满意度。结果中青年组的治疗总依从性(95.00%)与老年组(91.67%)比较差异无统计学意义(P>0.05);与干预前比较,干预后2组的SBP、DBP均显著降低(P<0.05),但组间比较差异无统计学意义(P>0.05);干预后2组的HAMA、HAMD评分均显著降低,且中青年组的HAMA、HAMD评分均低于老年组(P<0.05);干预后2组的共情能力、生活质量评分均显著升高,且中青年组的评分高于老年组(P<0.05);中青年组的满意度(93.33%)与老年组(86.67%)比较差异无统计学意义(P>0.05)。结论帕罗西汀联合共情技术应用于高血压合并焦虑抑郁患者,可促使患者积极配合治疗,有效控制血压,改善患者的焦虑抑郁情绪,提高患者的共情能力及生活质量,且患者满意度良好。中青年患者焦虑抑郁、共情能力及生活质量的改善情况优于老年患者。

按需服用Tramadol与日服Paroxetine哪一个更适合终身服用治疗早泄呢?

早泄是最常见的男性性功能障碍之一。目前临床上具有多种治疗方法，但临床效果极富争议。Paroxetine和tramadolHCl是目前治疗该病比较有效的药物。本文献就这两种药物（每日服用Paroxetine还是按需服用tramadolHCl的疗效做比较，以看哪一种更适合作为一种终身治疗早泄药物。以IELT（阴道内射精时间）和AIPE（早泄指数）来评估药物疗效。研究对象是取Mansoura大学医院在2008年4月至2009年3月参加男性学协会的患有早泄的患者。患者均经过严格筛选，需满足8项标准（参照文献）才能纳入研究。最后35例患者纳入研究。其中17例患者使用tramadolHCl，采用按需给药，临床观察前2-3h使用药物50mg；另外18例患者使用Paroxetine，采用每日给药，每日早餐后使用药物20mg。治疗周期为两个阶段，每个阶段六周，两个阶段治疗药物相同。

帕罗西汀致持续性呃逆1例

惊恐障碍患者在使用抗抑郁药时,可能会出现持续性呃逆,给患者带来严重痛苦。本文报道1例患有惊恐障碍的成年患者,接受了帕罗西汀、劳拉西泮和普萘洛尔治疗。住院第3天,帕罗西汀增加至30 mg/d,5 d后增加至40 mg/d,次日患者开始呃逆。将帕罗西汀剂量降至30 mg/d,同时予以氯丙嗪改善呃逆表现,4 d后患者呃逆停止。根据病情需要,将帕罗西汀剂量增加至40 mg/d,患者再次出现呃逆,但与首次发作相比,持续时间较短,且严重程度较轻。再次给予氯丙嗪对症治疗,呃逆症状持续24 h后不再出现。帕罗西汀维持在40 mg/d,直至出院未再出现呃逆。帕罗西汀可引起成人惊恐障碍患者急性给药期持续性呃逆,应引起关注。

盐酸帕罗西汀片联合四联疗法对幽门螺旋杆菌相关慢性胃炎合并抑郁患者的临床疗效

目的:探讨幽门螺杆菌(HP)相关慢性胃炎合并抑郁患者在四联疗法的基础上配合盐酸帕罗西汀片治疗的临床效果。方法:以112例HP相关慢性胃炎合并抑郁患者为研究对象,按不同治疗方案分为对照组(接受常规四联疗法)与观察组(合用盐酸帕罗西汀片),每组各56例。比较两组患者焦虑抑郁程度、临床疗效、HP清除率、生活质量。结果:治疗后,两组汉密尔顿焦虑量表(HAMA)、汉密尔顿抑郁量表(HAMD)评分均降低,且观察组低于对照组(P<0.05);观察组患者临床总疗效高于对照组(P<0.05);观察组HP根除率高于对照组(P<0.05);治疗后,两组患者简明健康状况调查量表(SF-36)测评结果均升高,且观察组高于对照组(P<0.05)。结论:盐酸帕罗西汀片联合四联疗法治疗HP相关慢性胃炎合并抑郁患者,可减轻焦虑抑郁程度,以增强疗效,提高HP清除率,起到改善患者生活质量的积极作用。

疏肝通络针刺法联合帕罗西汀治疗卒中后抑郁症临床疗效及对神经递质、细胞因子表达水平的影响

目的通过随机对照研究,研究疏肝通络针刺法联合帕罗西汀治疗卒中后抑郁症(PSD)患者的临床疗效观察及对神经递质、细胞因子表达水平的影响。方法利用随机数字表法将医院2022年7月—2023年1月收治的90例PSD患者分为研究组(45例,疏肝通络针刺法+帕罗西汀)和对照组(45例,帕罗西汀);对比两组临床疗效,治疗前后抑郁情况[抑郁自评量表(SDS)、汉密尔顿抑郁量表(HAMD)]、生活质量,治疗前后神经递质[同型半胱胺酸(Hcy)、5-羟色胺(5-HT)、多巴胺(DA)、去甲肾上腺素(NA)]、细胞因子[白细胞介素-1(IL-1)、白细胞介素-10(IL-10)、肿瘤坏死因子-α(TNF-α)]等水平,记录不良反应情况。结果治疗8周后,总有效率研究组高于对照组(P<0.05);两组HAMD、SDS评分均下降(P<0.05),且研究组均低于对照组(P<0.05);研究组生活质量量表评分均高于对照组和治疗前(P<0.05);两组Hcy、IL-1、TNF-α均降低,且研究组低于对照组(P<0.05);两组5-HT、DA、NA及IL-10均升高(P<0.05),且研究组均高于对照组(P<0.05);研究组不良反应总发生率低于对照组(4.44%vs 17.78%,χ^(2)=4.050,P<0.05)。结论对PSD患者给予疏肝通络针刺法联合帕罗西汀治疗,可获得更好地治疗效果,可有效缓解患者抑郁情绪,调节神经递质、细胞因子水平,且不良反应较少。

牡蛎肽对帕罗西汀致雄性小鼠性功能障碍的作用效果及潜在机制

牡蛎肽(Oyster peptide,OP)具有多种生物活性,然而,其对男性性功能障碍的作用效果仍知之甚少。以牡蛎肽为研究对象,探讨其对男性性功能障碍的作用效果及其潜在机制。每天灌胃帕罗西汀(Paroxetine,PRX)构建雄性小鼠性功能障碍模型,同时灌胃牡蛎肽(500 mg·kg^(−1)),持续28 d。结果表明:与模型(PRX)组小鼠相比,牡蛎肽可显著提高雄性小鼠的性能力(P<0.05),恢复血清性激素水平(P<0.01),提高阴茎组织一氧化氮(NO)含量(P<0.01)、环磷酸鸟苷(cGMP)含量(P<0.05),和一氧化氮合酶(NOS)活性(P<0.05),并降低磷酸二酯酶-5(PDE-5)活性(P<0.01);同时,牡蛎肽可增强睾丸标志性酶活性(P<0.05)和抗氧化能力(P<0.01),改善精子质量。此外,HE染色结果显示:牡蛎肽可恢复小鼠睾丸生精小管内生精细胞的数量与形态,减少生精小管空泡化现象。综上所述,牡蛎肽可有效减缓PRX导致的雄性小鼠性功能障碍,推测其对男性性功能障碍具有潜在的保护作用。