Loy Jik H, Merry Sally N, Hetrick Sarah E, Stasiak Karolina
Child and Adolescent Mental Health, Health Waikato, Hamilton, New Zealand.
Cochrane Database Syst Rev. 2012 Sep 12(9):CD008559. doi: 10.1002/14651858.CD008559.pub2.
Disruptive behaviour disorders include conduct disorder, oppositional defiant disorder and disruptive behaviour not otherwise specified. Attention deficit hyperactivity disorder (ADHD) is frequently associated with disruptive behaviour disorders. The difficulties associated with disruptive behaviour disorders are demonstrated through aggression and severe behavioural problems. These often result in presentation to psychiatric services and may be treated with medications such as atypical antipsychotics. There is increasing evidence of a significant rise in the use of atypical antipsychotics for treating disruptive behaviour disorders in child and adolescent populations.
To evaluate the effect and safety of atypical antipsychotics, compared to placebo, for treating disruptive behaviour disorders in children and youths.
We searched the following databases in August 2011: CENTRAL (2011, Issue 3), MEDLINE (1948 to August Week 1), EMBASE (1980 to 2011 Week 32), PsycINFO (1806 to August Week 2 2011), CINAHL (1937 to current), ClinicalTrials.gov (searched 15 August 2011), Australian New Zealand Clinical Trials Registry (ANZCTR) (searched 15 August 2011), CenterWatch (searched 15 August 2011) and ICTRP (searched 15 August 2011).
We included randomised controlled trials with children and youths up to and including the age of 18, in any setting, with a diagnosis of a disruptive behaviour disorder. We included trials where participants had a comorbid diagnosis of attention deficit hyperactivity disorder, major depression or an anxiety disorder.
Two review authors independently selected the studies and disagreements were resolved by discussion. Two review authors extracted data independently. One review author entered data into Review Manager software and another checked it. We contacted trial authors for information about adverse effects and to provide missing data.
We included eight randomised controlled trials, spanning 2000 to 2008. Seven assessed risperidone and one assessed quetiapine. Three of the studies were multicentre. Seven trials assessed acute efficacy and one assessed time to symptom recurrence over a six-month maintenance period.We performed meta-analyses for the primary outcomes of aggression, conduct problems and weight changes but these were limited by the available data as different trials reported either mean change scores (average difference) or final/post-intervention raw scores and used different outcome measures. We also evaluated each individual trial's treatment effect size where possible, using Hedges' g.For aggression, we conducted two meta-analyses. The first included three trials (combined n = 238) using mean difference (MD) on the Aberrant Behaviour Checklist (ABC) Irritability subscale. Results yielded a final mean score with treatment that was 6.49 points lower than the post-intervention mean score with placebo (95% confidence interval (CI) -8.79 to -4.19). The second meta-analysis on aggression included two trials (combined n = 57) that employed two different outcome measures (Overt Aggression Scale (modified) (OAS-M) and OAS, respectively) and thus we used a standardised mean difference. Results yielded an effect estimate of -0.18 (95% CI -0.70 to 0.34), which was statistically non-significant.We also performed two meta-analyses for conduct problems. The first included two trials (combined n = 225), both of which employed the Nisonger Child Behaviour Rating Form - Conduct Problem subscale (NCBRF-CP). The results yielded a final mean score with treatment that was 8.61 points lower than that with placebo (95% CI -11.49 to -5.74). The second meta-analysis on conduct problems included two trials (combined n = 36), which used the Conners' Parent Rating Scale - Conduct Problem subscale (CPRS-CP). Results yielded a mean score with treatment of 12.67 lower than with placebo (95% CI -37.45 to 12.11), which was a statistically non-significant result.With respect to the side effect of weight gain, a meta-analysis of two studies (combined n = 138) showed that participants on risperidone gained on average 2.37 kilograms more than those in the placebo group over the treatment period (MD 2.37; 95% CI 0.26 to 4.49).For individual trials, there was a range of effect sizes (ranging from small to large) for risperidone reducing aggression and conduct problems. The precision of the estimate of the effect size varied between trials.
AUTHORS' CONCLUSIONS: There is some limited evidence of efficacy of risperidone reducing aggression and conduct problems in children aged 5 to 18 with disruptive behaviour disorders in the short term.For aggression, the difference in scores of 6.49 points on the ABC Irritability subscale (range 0 to 45) may be clinically significant. For conduct problems, the difference in scores of 8.61 points on the NCBRF-CP (range 0 to 48) is likely to be clinically significant.Caution is required due to the limitations of the evidence and the small number of relevant high-quality studies. The findings from the one study assessing impact in the longer term suggest that the effects are maintained to some extent (small effect size) for up to six months. Inadequately powered studies produced non-significant results. The evidence is restricted by heterogeneity of the population (including below average and borderline IQ), and methodological issues in some studies, such as use of enriched designs and risk of selection bias. No study addressed the issue of pre-existing/concurrent psychosocial interventions, and comorbid stimulant medication and its dosage was only partially addressed. There is currently no evidence to support the use of quetiapine for disruptive behaviour disorders in children and adolescents.It is uncertain to what degree the efficacy found in clinical trials will translate into real life clinical practice. Participants in the studies were recruited from clinical services but those who agree to take part in the clinical trials are a subset of the overall population presenting for care. There are no research data for children under five years of age. Further high-quality research is required with large samples of clinically representative youths and long-term follow-up to replicate current findings.
破坏性行为障碍包括品行障碍、对立违抗障碍以及未另行规定的破坏性行为。注意力缺陷多动障碍(ADHD)常与破坏性行为障碍相关。破坏性行为障碍所带来的困难通过攻击行为和严重行为问题得以体现。这些情况常常导致患者就诊于精神科服务机构,并且可能会使用非典型抗精神病药物等进行治疗。越来越多的证据表明,在儿童和青少年人群中,使用非典型抗精神病药物治疗破坏性行为障碍的情况显著增加。
与安慰剂相比,评估非典型抗精神病药物治疗儿童和青少年破坏性行为障碍的疗效和安全性。
我们于2011年8月检索了以下数据库:Cochrane系统评价数据库(CENTRAL,2011年第3期)、医学索引数据库(MEDLINE,1948年至2011年第33周)、荷兰医学文摘数据库(EMBASE,1980年至2011年第32周)、心理学文摘数据库(PsycINFO,1806年至2011年第33周)、护理学与健康领域数据库(CINAHL,1937年至今)、临床试验注册库(ClinicalTrials.gov,检索日期为2011年8月15日)、澳大利亚和新西兰临床试验注册中心(ANZCTR,检索日期为2011年8月15日)、CenterWatch(检索日期为2011年8月15日)以及国际临床试验注册平台(ICTRP,检索日期为2011年8月15日)。
我们纳入了在任何环境下针对年龄在18岁及以下、诊断为破坏性行为障碍的儿童和青少年进行的随机对照试验。我们纳入了参与者同时患有注意力缺陷多动障碍、重度抑郁症或焦虑症的试验。
两名综述作者独立选择研究,分歧通过讨论解决。两名综述作者独立提取数据。一名综述作者将数据录入Review Manager软件,另一名作者进行核对。我们联系试验作者获取有关不良反应的信息并补充缺失数据。
我们纳入了8项随机对照试验,时间跨度为2000年至2008年。7项评估了利培酮,1项评估了喹硫平。其中3项研究为多中心研究。7项试验评估了急性疗效,1项评估了为期6个月维持期内症状复发的时间。我们对攻击行为、品行问题和体重变化等主要结局进行了荟萃分析,但这些分析受到可用数据的限制,因为不同试验报告的要么是平均变化分数(平均差值),要么是干预后最终/原始分数,且使用了不同的结局测量方法。我们还在可能的情况下,使用Hedges' g评估了每个单独试验的治疗效应大小。对于攻击行为,我们进行了两项荟萃分析。第一项纳入了3项试验(合并样本量n = 238),使用异常行为检查表(ABC)易激惹分量表上的平均差值(MD)。结果显示,治疗后的最终平均分数比安慰剂干预后的平均分数低6.49分(95%置信区间(CI)-8.79至-4.19)。第二项关于攻击行为的荟萃分析纳入了2项试验(合并样本量n = 57),这两项试验分别采用了两种不同的结局测量方法(分别为改良版公开攻击量表(OAS-M)和公开攻击量表(OAS)),因此我们使用了标准化平均差值。结果得出的效应估计值为-0.18(95% CI -0.70至0.34),在统计学上无显著意义。我们还对品行问题进行了两项荟萃分析。第一项纳入了2项试验(合并样本量n = 225),这两项试验均采用了尼桑格儿童行为评定量表 - 品行问题分量表(NCBRF-CP)。结果显示,治疗后的最终平均分数比安慰剂组低8.
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