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Clinical value of early partial symptomatic improvement in the prediction of response and remission during short-term treatment trials in 3369 subjects with bipolar I or II depression

机译:在3369例双相I型或II型抑郁症患者的短期治疗试验中,早期部分症状改善对缓解和缓解的预测的临床价值

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摘要

OBJECTIVE: To evaluate the clinical value of early partial symptomatic improvement in predicting the probability of response during the short-term treatment of bipolar depression. METHODS: Blinded data from 10 multicenter, randomized, double-blind, placebo-controlled trials in bipolar I or II depression were used to determine if early improvement (≥20% reduction in depression symptom severity after 14days of treatment) predicted later short-term response or remission. Sensitivity, specificity, efficiency, and positive and negative predictive values (PPV, NPV) were calculated using an intent to treat analysis of individual and pooled study data. RESULTS: 1913 patients were randomized to active compounds (aripiprazole, lamotrigine, olanzapine/olanzapine-fluoxetine, and quetiapine), and 1456 to placebo. In the pooled positive studies, early improvement predicted response and remission with high sensitivity (86% and 88%, respectively), but rates of false positives were high (53% and 59%, respectively). Pooled negative predictive values for response/remission (i.e. confidence in knowing the drug will not result in response or remission) were 74% and 82%, respectively, with low rates of false negatives (14% and 12%, respectively). CONCLUSION: Early improvement in an individual patient does not appear to be a reliable predictor of eventual response or remission due to an unacceptably high false positive rate. However, the absence of early improvement appears to be a highly reliable predictor of eventual non-response, suggesting that clinicians can have confidence in knowing when a drug is not going to work during short-term treatment. Patients who fail to demonstrate early improvement within the first two weeks of treatment may benefit from a change in therapy.
机译:目的:评估早期局部症状改善在预测双相抑郁症短期治疗期间的反应可能性方面的临床价值。方法:使用来自10项双中心I型或II型抑郁症的多中心,随机,双盲,安慰剂对照试验的盲数据,来确定早期改善(治疗14天后抑郁症状严重程度降低≥20%)是否预测了以后的短期治疗反应或缓解。敏感性,特异性,效率以及阳性和阴性预测值(PPV,NPV)的计算旨在处理对单个和汇总研究数据的分析。结果:1913例患者被随机分配至活性化合物(阿立哌唑,拉莫三嗪,奥氮平/奥氮平-氟西汀和喹硫平),而1456例患者被随机分配至安慰剂。在汇总的阳性研究中,早期改善以高敏感性预测了缓解和缓解(分别为86%和88%),但假阳性率很高(分别为53%和59%)。对于缓解/缓解的总阴性预测值(即对了解药物不会导致缓解或缓解的信心)分别为74%和82%,假阴性率较低(分别为14%和12%)。结论:由于假阳性率高得令人无法接受,因此单个患者的早期改善似乎不是可靠的预测最终反应或缓解的指标。但是,缺乏早期改善似乎是最终无反应的高度可靠的预测指标,这表明临床医生可以对短期治疗期间什么时候药物无效没有信心。在治疗的前两周内未能显示出早期改善的患者可能会从治疗改变中受益。

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