CPS Research, Glasgow, Scotland, UK.
Psychol Med. 2011 Oct;41(10):2089-97. doi: 10.1017/S0033291711000158. Epub 2011 Feb 25.
Selective serotonin reuptake inhibitors take several weeks to achieve their full antidepressant effects. Post-synaptic 5-HT2A receptor activation is thought to be involved in this delayed therapeutic effect. Pipamperone acts as a highly selective 5-HT2A/D4 antagonist when administered in low doses. The purpose of this study was to compare citalopram 40 mg once daily plus pipamperone 5 mg twice daily (PipCit) versus citalopram plus placebo twice daily for magnitude and onset of therapeutic effect.
An 8-week, randomized, double-blind study in patients with major depressive disorder was carried out.
The study population comprised 165 patients (citalopram and placebo, n=82; PipCit, n=83) with a mean baseline Montgomery-Asberg Depression Rating Scale (MADRS) score of 32.6 (s.d.=5.5). In the first 4 weeks, more citalopram and placebo than PipCit patients discontinued treatment (18% v. 4%, respectively, p=0.003). PipCit patients had significantly greater improvement in MADRS score at week 1 [observed cases (OC), p=0.021; last observation carried forward (LOCF), p=0.007] and week 4 (LOCF, p=0.025) but not at week 8 compared with citalopram and placebo patients. Significant differences in MADRS scores favoured PipCit in reduced sleep, reduced appetite, concentration difficulties and pessimistic thoughts. Mean Clinical Global Impression-Improvement scores were significantly improved after 1 week of PipCit compared with citalopram and placebo (OC and LOCF, p=0.002).
Although the MADRS score from baseline to 8 weeks did not differ between groups, PipCit provided superior antidepressant effects and fewer discontinuations compared with citalopram and placebo during the first 4 weeks of treatment, especially in the first week.
选择性 5-羟色胺再摄取抑制剂需要数周时间才能发挥其全部抗抑郁作用。人们认为,突触后 5-HT2A 受体的激活参与了这种延迟的治疗效果。哌泊噻嗪在低剂量下作为一种高度选择性的 5-HT2A/D4 拮抗剂。本研究旨在比较每日一次西酞普兰 40mg 加每日两次哌泊噻嗪 5mg(PipCit)与西酞普兰加每日两次安慰剂的疗效大小和起效时间。
一项为期 8 周的、随机的、双盲研究,纳入了患有重度抑郁症的患者。
研究人群包括 165 名患者(西酞普兰和安慰剂组,n=82;PipCit 组,n=83),他们的基线蒙哥马利-阿斯伯格抑郁评定量表(MADRS)评分平均为 32.6(标准差=5.5)。在前 4 周,与西酞普兰和安慰剂相比,更多的 PipCit 患者停止了治疗(分别为 18%和 4%,p=0.003)。与西酞普兰和安慰剂相比,PipCit 患者在第 1 周[观察病例(OC),p=0.021;最后一次观察向前传递(LOCF),p=0.007]和第 4 周(LOCF,p=0.025)的 MADRS 评分有显著改善,但在第 8 周时没有显著改善。在减少睡眠、减少食欲、注意力困难和悲观思维方面,MADRS 评分的显著改善对 PipCit 有利。与西酞普兰和安慰剂相比,PipCit 在第 1 周时的平均临床总体印象-改善评分有显著改善(OC 和 LOCF,p=0.002)。
尽管从基线到 8 周时,各组之间的 MADRS 评分没有差异,但与西酞普兰和安慰剂相比,PipCit 在治疗的前 4 周提供了更好的抗抑郁作用和更少的停药率,尤其是在第 1 周。
