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首页> 外文期刊>Molecular Psychiatry >Effects of immunomodulatory drugs on depressive symptoms: A mega-analysis of randomized, placebo-controlled clinical trials in inflammatory disorders
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Effects of immunomodulatory drugs on depressive symptoms: A mega-analysis of randomized, placebo-controlled clinical trials in inflammatory disorders

机译:免疫调节药对抑郁症状的影响:炎症性障碍随机,安慰剂对照试验的兆分析

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摘要

Activation of the innate immune system is commonly associated with depression. Immunomodulatory drugs may have efficacy for depressive symptoms that are co-morbidly associated with inflammatory disorders. We report a large-scale re-analysis by standardized procedures (mega-analysis) of patient-level data combined from 18 randomized clinical trials conducted by Janssen or GlaxoSmithKline for one of nine disorders (N-=-10,743 participants). Core depressive symptoms (low mood, anhedonia) were measured by the Short Form Survey (SF-36) or the Hospital Anxiety and Depression Scale (HADS), and participants were stratified into high (N-=-1921) versus low-depressive strata based on baseline ratings. Placebo-controlled change from baseline after 4-16 weeks of treatment was estimated by the standardized mean difference (SMD) over all trials and for each subgroup of trials targeting one of 7 mechanisms (IL-6, TNF-α, IL-12/23, CD20, COX2, BLγS, p38/MAPK14). Patients in the highdepressive stratum showed modest but significant effects on core depressive symptoms (SMD-=-0.29, 95% CI [0.12-0.45]) and related SF-36 measures of mental health and vitality. Anti-IL-6 antibodies (SMD-=-0.8, 95% CI [0.20-1.41]) and an anti-IL-12/23 antibody (SMD-=-0.48, 95% CI [0.26-0.70]) had larger effects on depressive symptoms than other drug classes. Adjustments for physical health outcome marginally attenuated the average treatment effect on depressive symptoms (SMD-=-0.20, 95% CI: 0.06-0.35), but more strongly attenuated effects on mental health and vitality. Effects of anti-IL-12/23 remained significant and anti-IL-6 antibodies became a trend after controlling for physical response to treatment. Novel immune-therapeutics can produce antidepressant effects in depressed patients with primary inflammatory disorders that are not entirely explained by treatment-related changes in physical health.
机译:先天免疫系统的激活通常与抑郁症有关。免疫调节药物可能具有与炎症疾病有关的抑郁症状的疗效。我们通过标准化程序(兆分析)的患者级数据进行了大规模的重新分析,所述患者水平数据组合于Janssen或Glaxosmithkline的18项随机临床试验,适用于九个疾病之一(n - = - 10,743名参与者)。通过短的形式测量(SF-36)或医院焦虑和抑郁尺度(HAFS)测量核心抑郁症状(低情,Anhedonia),参与者分为高(N - = - 1921)与低抑郁阶层基于基线等级。通过所有试验的标准化平均差(SMD)估算4-16周的基线的安慰剂控制的变化,并针对靶向7种机制中的一种试验亚组(IL-6,TNF-α,IL-12 / 23,CD20,COX2,BLγS,P38 / MAPK14)。患者在高级抑郁层中表现出适度但对核心抑郁症状的显着影响(SMD - = - 0.29,95%CI [0.12-0.45])和相关的SF-36心理健康和活力措施。抗IL-6抗体(SMD - = - 0.8,95%CI [0.20-1.41])和抗IL-12/23抗体(SMD - = - 0.48,95%CI [0.26-0.70])具有更大的对抑郁症状的影响比其他药物课程。身体健康结果的调整略微减弱了对抑郁症状的平均治疗效果(SMD - = - 0.20,95%CI:0.06-0.35),但对心理健康和活力的影响更大。抗IL-12/23的效果仍然是显着的,抗IL-6抗体在控制对治疗的物理反应后成为趋势。新型免疫治疗剂可以产生抑郁症患者的抑郁症患者,其初发性炎症障碍不完全由身体健康的治疗相关变化进行完全解释。

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