New York Medical College, Valhalla, NY, USA.
Int J Clin Pract. 2012 Apr;66(4):356-68. doi: 10.1111/j.1742-1241.2011.02885.x. Epub 2012 Jan 29.
To describe the efficacy and safety of vilazodone for the treatment of major depressive disorder (MDD).
The pivotal registration trials were accessed by querying http://www.ncbi.nlm.nih.gov/pubmed/, http://www.fda.gov and http://www.clinicaltrials.gov for the search term 'vilazodone'. Product labeling provided additional information.
All available clinical reports of studies were identified.
Descriptions of the principal results and calculation of number needed to treat (NNT) and number needed to harm (NNH) for relevant dichotomous outcomes were extracted from the available study reports and other sources of information.
Vilazodone is a specific serotonin reuptake inhibitor and serotonin 5HT1A receptor partial agonist. In needs to be administered with food to ensure adequate bioavailability. Approval for the treatment of MDD was based on a clinical development programme that included two 8-week placebo-controlled randomised clinical trials in outpatients with MDD where vilazodone was titrated to a target dose of 40 mg/d over the first 2 weeks. Both trials evidenced efficacy for vilazodone as measured by the Montgomery Asberg Depression Rating Scale. NNT for response vs. placebo was 8 (95% CI 6-16) and for remission was 14 (95% CI 8-55). NNH vs. placebo for discontinuation because of an adverse event (AE) was 27 (95% CI 15-104). The most commonly encountered AEs (incidence ≥ 5% and at least twice the rate of placebo) were diarrhoea, nausea, vomiting and insomnia, with NNH values vs. placebo of 6 (95% CI 5-8), 6 (95% CI 5-8), 30 (95% CI 18-82) and 26 (95% CI 16-78), respectively. NNH vs. placebo for any sexual AE was 12 (95% CI 9-18), but systematically collected data using rating scales of sexual function did not reveal treatment associated effects. Vilazodone was not associated with clinically relevant weight change in the short-term trials. In an open-label 1-year study of vilazodone, mean weight increased by 1.7 kg among the observed cases.
Vilazodone represents another option for the treatment of MDD. Vilazodone appears to have a favourable weight-gain profile based on short-term studies. Sexual side-effects were not consistently demonstrated when assessed using clinical rating scales but spontaneously reported AEs related to sexual functioning were observed. Additional controlled data regarding long-term efficacy and effectiveness will help characterise this new agent when used in maintenance treatment.
描述维拉佐酮治疗重度抑郁症(MDD)的疗效和安全性。
通过在 http://www.ncbi.nlm.nih.gov/pubmed/、http://www.fda.gov 和 http://www.clinicaltrials.gov 上搜索“维拉佐酮”来检索关键注册试验。产品标签提供了额外的信息。
确定了所有可用的研究临床报告。
从可用的研究报告和其他信息来源中提取主要结果描述和计算相关二分类结局的需要治疗人数(NNT)和需要损害人数(NNH)。
维拉佐酮是一种特异性 5-羟色胺再摄取抑制剂和 5-羟色胺 1A 受体部分激动剂。为确保充分的生物利用度,需要与食物一起给药。MDD 的批准是基于一项临床开发计划,该计划包括两项为期 8 周的安慰剂对照随机临床试验,在门诊 MDD 患者中,维拉佐酮在最初的 2 周内滴定至目标剂量 40mg/d。两项试验均证明了维拉佐酮的疗效,以蒙哥马利抑郁评定量表(MADRS)测量。与安慰剂相比,反应的 NNT 为 8(95%CI 6-16),缓解的 NNT 为 14(95%CI 8-55)。与安慰剂相比,因不良事件(AE)而停药的 NNH 为 27(95%CI 15-104)。最常见的不良事件(发生率≥5%且至少是安慰剂的两倍)为腹泻、恶心、呕吐和失眠,与安慰剂相比的 NNH 值分别为 6(95%CI 5-8)、6(95%CI 5-8)、30(95%CI 18-82)和 26(95%CI 16-78)。与安慰剂相比,任何性 AE 的 NNH 为 12(95%CI 9-18),但使用性功能评分量表系统收集的数据并未显示治疗相关的影响。维拉佐酮在短期试验中与体重的临床相关变化无关。在维拉佐酮为期 1 年的开放标签研究中,观察病例的平均体重增加了 1.7kg。
维拉佐酮为 MDD 的治疗提供了另一种选择。基于短期研究,维拉佐酮似乎具有有利的体重增加特征。使用临床评分量表评估时并未一致显示出性副作用,但观察到与性功能相关的自发报告 AE。关于长期疗效和有效性的额外对照数据将有助于描述该新药物在维持治疗中的作用。
