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预防儿童和青少年抑郁症的心理和/或教育干预措施。

Psychological and/or educational interventions for the prevention of depression in children and adolescents.

作者信息

Merry S, McDowell H, Hetrick S, Bir J, Muller N

机构信息

Department of Psychiatry, University of Auckland, Private Bag 92019, Auckland, New Zealand.

出版信息

Cochrane Database Syst Rev. 2004(1):CD003380. doi: 10.1002/14651858.CD003380.pub2.

Abstract

BACKGROUND

Depression is the fourth most important disease in the estimation of the burden of disease Murray 1996 and is a common problem with prevalence rates estimated to be as high as 8% in young people. Depression in young people is associated with poor academic performance, social dysfunction, substance abuse, suicide attempts, and completed suicide (NHMRC 1997). This has precipitated the development of programmes aimed at preventing the onset of depression. This review evaluates evidence for the effectiveness of these prevention programmes.

OBJECTIVES

To determine whether psychological and/or educational interventions (both universal and targeted) are effective in reducing risk of depressive disorder by reducing depressive symptoms immediately after intervention or by preventing the onset of depressive disorder in children and adolescents over the next one to three years.

SEARCH STRATEGY

The Cochrane Depression, Anxiety and Neurosis Group trials register (August 2002), MEDLINE (1966 to December Week 3 2002), EMBASE (1980 to January Week 2 2003), PsychInfo (1886 to January Week 2 2003) and ERIC (1985 to December 2002) were searched. In addition, conference abstracts, the reference lists of included studies, and other reviews were searched and experts in the field were contacted.

SELECTION CRITERIA

Each identified study was assessed for possible inclusion by two independent reviewers based on the methods sections. The determinants for inclusion were that the trial include a psychological and/or educational prevention programme for young people aged 5 to 19 years-old, who did not meet DSM or ICD criteria for depression and/or did not fall into the clinical range on standardised, validated, and reliable rating scales of depression.

DATA COLLECTION AND ANALYSIS

The methodological quality of the included trials was assessed by two independent reviewers according to a list of pre-determined criteria, which were based on quality ratings devised by Moncrieff and colleagues (Moncrieff 2001). Outcome data was extracted and entered into Revman 4.2. Means and standard deviations for continuous outcomes and number of events for dichotomous outcomes were extracted where available. For trials where the required data were not reported or could not be calculated, further details were requested from first authors. If no further details were provided, the trial was included in the review and described, but not included in the meta-analysis. Results were presented for each type of intervention: targeted or universal interventions; and educational or psychological interventions and if data were provided, by gender. Where possible data were combined in meta-analyses to give a treatment effect across all trials. Sensitivity analysis were conducted on studies rated as "adequate" or "high" quality, that is with a score over 22, based on the scale by Moncrieff et al (Moncrieff 2001). The presence of publication bias was assessed using funnel plots.

MAIN RESULTS

Studies were divided into those that compared intervention with an active comparison or placebo (i.e. a control condition that resembles the intervention being investigated but which lacks the elements thought to be active in preventing depression) and those that used a "wait-list" or no intervention comparison group. Only two studies fell into the former category and neither showed effectiveness although one study was inadequately powered to show a difference and in the other the "placebo" contained active therapeutic elements, reducing the ability to demonstrate a difference from intervention. Psychological interventions were effective compared with non-intervention immediately after the programmes were delivered with a significant reduction in scores on depression rating scales for targeted (standardised mean difference (SMD) of -0.26 and a 95% confidence interval (CI) of -0.40 to -0.13 ) but not universal interventions (SMD -0.21, 95% CI -0.48, 0.06), with a significant effect maintained on pooling data (SMD -0.26, 95% CI -0.36, -0.15). While small effect sizes were reported, these were associated with a significant reduction in depressive episodes. The overall risk difference after intervention translates to "numbers needed to treat" (NNT) of 10. The most effective study is the targeted programme by Clarke (Clarke 2001) where the initial effect size of -0.46 is associated with an initial risk difference of -0.22 and NNT 5. There was no evidence of effectiveness for educational interventions. Reports of effectiveness for boys and girls were contradictory. The quality of many studies was poor, and only two studies made allocation concealment explicit. Sensitivity analysis of only high quality studies did not alter the results significantly. The only analysis in which there was significant statistical heterogeneity was the sub-group analysis by gender where there was variability in the response to different programmes for both girls and boys. For the most part funnel plots indicate findings are robust for short term effects with no publication bias evident. There are too few studies to comment on whether there is publication bias for studies reporting long-term (12-36 month) follow-up.

REVIEWER'S CONCLUSIONS: Although there is insufficient evidence to warrant the introduction of depression prevention programmes currently, results to date indicate that further study would be worthwhile. There is a need to compare interventions with a placebo or some sort of active comparison so that study participants do not know whether they are in the intervention group or not, to investigate the impact of booster sessions to see if effectiveness immediately after intervention can be prolonged, ideally for a year or longer, and to consider practical implementation of prevention programmes when choosing target populations. Until now most studies have focussed on psychological interventions. The potential effectiveness of educational interventions has not been fully investigated. Given the gender differences in prevalence, and the change in these that occurs in adolescence with a disproportionate increase in prevalence rates for girls, it is likely that girls and boys will respond differently to interventions. Although differences have been reported in studies in this review the findings are contradictory and a more definitive delineation of gender specific responses to interventions would be helpful.

摘要

背景

在1996年默里对疾病负担的评估中,抑郁症是第四大重要疾病,是一个普遍问题,据估计,年轻人中的患病率高达8%。年轻人的抑郁症与学业成绩差、社交功能障碍、药物滥用、自杀未遂和自杀(澳大利亚国家卫生与医学研究委员会,1997年)有关。这促使了旨在预防抑郁症发作的项目的发展。本综述评估了这些预防项目有效性的证据。

目的

确定心理和/或教育干预措施(包括普遍干预和针对性干预)是否能通过在干预后立即减轻抑郁症状或在未来一至三年内预防儿童和青少年抑郁症的发作,有效降低抑郁症的风险。

检索策略

检索了Cochrane抑郁症、焦虑症和神经症小组试验注册库(2002年8月)、MEDLINE(1966年至2002年12月第3周)、EMBASE(1980年至2003年1月第2周)、PsychInfo(1886年至2003年1月第2周)和ERIC(1985年至2002年12月)。此外,还检索了会议摘要、纳入研究的参考文献列表和其他综述,并联系了该领域的专家。

选择标准

两名独立评审员根据方法部分对每项识别出的研究进行评估,以确定是否可能纳入。纳入的决定因素是,试验包括针对5至19岁未符合抑郁症DSM或ICD标准且在标准化、经过验证且可靠的抑郁症评定量表上未处于临床范围的年轻人的心理和/或教育预防项目。

数据收集与分析

两名独立评审员根据预先确定的标准列表对纳入试验的方法学质量进行评估,这些标准基于蒙克里夫及其同事制定的质量评级(蒙克里夫,2001年)。提取结果数据并输入Revman 4.2。在可行的情况下,提取连续结果的均值和标准差以及二分结果的事件数。对于未报告所需数据或无法计算所需数据的试验,向第一作者索要进一步的详细信息。如果没有提供进一步的详细信息,则将该试验纳入综述并进行描述,但不纳入荟萃分析。针对每种干预类型呈现结果:针对性干预或普遍干预;教育干预或心理干预,并在提供数据时按性别呈现。在可能的情况下,将数据合并进行荟萃分析,以得出所有试验的治疗效果。对评为“充分”或“高质量”(即根据蒙克里夫等人的量表得分超过22分)的研究进行敏感性分析(蒙克里夫,2001年)。使用漏斗图评估发表偏倚的存在情况。

主要结果

研究分为将干预与积极对照或安慰剂进行比较的研究(即一种对照条件,类似于所研究的干预措施,但缺乏被认为对预防抑郁症有积极作用的要素)以及使用“等待列表”或无干预比较组的研究。只有两项研究属于前一类,且均未显示出有效性,尽管一项研究的样本量不足以显示差异,而另一项研究中的“安慰剂”包含积极的治疗要素,降低了显示与干预差异的能力。与不干预相比,心理干预在项目实施后立即有效,针对性干预在抑郁症评定量表上的得分显著降低(标准化均数差(SMD)为 -0.26,95%置信区间(CI)为 -0.40至 -0.13),但普遍干预则不然(SMD -0.21,95% CI -0.48,0.06),汇总数据时仍有显著效果(SMD -0.26,95% CI -0.36, -0.15)。虽然报告的效应量较小,但与抑郁发作的显著减少相关。干预后的总体风险差异转化为“需治疗人数”(NNT)为10。最有效的研究是克拉克的针对性项目(克拉克,2001年),其初始效应量为 -0.46,初始风险差异为 -0.22,NNT为5。没有证据表明教育干预有效。关于男孩和女孩有效性的报告相互矛盾。许多研究的质量较差,只有两项研究明确说明了分配隐藏情况。仅对高质量研究进行的敏感性分析并未显著改变结果。唯一存在显著统计异质性的分析是按性别进行的亚组分析,其中女孩和男孩对不同项目的反应存在差异。在大多数情况下,漏斗图表明短期效应的结果是可靠的,没有明显的发表偏倚。对于报告长期(12 - 36个月)随访的研究,由于研究数量过少,无法评论是否存在发表偏倚。

综述作者结论

尽管目前没有足够的证据支持引入抑郁症预防项目,但迄今为止的结果表明进一步研究是值得的。需要将干预措施与安慰剂或某种积极对照进行比较,以便研究参与者不知道自己是否在干预组中;需要研究强化疗程的影响,以确定干预后立即出现的有效性是否可以延长,理想情况下延长一年或更长时间;在选择目标人群时需要考虑预防项目的实际实施情况。到目前为止,大多数研究都集中在心理干预上。教育干预的潜在有效性尚未得到充分研究。鉴于患病率存在性别差异,且在青春期这种差异会发生变化,女孩的患病率不成比例地增加,男孩和女孩可能对干预有不同的反应。尽管本综述中的研究报告了差异,但结果相互矛盾,更明确地界定性别对干预的特定反应将有所帮助。

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