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首页> 外文期刊>Neurotoxicity research >Add-on Treatment with Curcumin Has Antidepressive Effects in Thai Patients with Major Depression: Results of a Randomized Double-Blind Placebo-Controlled Study
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Add-on Treatment with Curcumin Has Antidepressive Effects in Thai Patients with Major Depression: Results of a Randomized Double-Blind Placebo-Controlled Study

机译:姜黄素的附加治疗在泰国患者的主要抑郁症患者中具有抗癌效应:随机双盲安慰剂对照研究的结果

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Abstract Activation of immune-inflammatory and oxidative-nitrosative (IO&NS) stress pathways plays a role in major depression (MDD). Evidence suggests that curcumin (500–1000?mg/day), a polyphenol with strong anti-IO&NS properties, may have efficacy either as monotherapy or as an adjunctive treatment for depression. Further controlled trials with extended treatment periods (>?8?weeks) and higher curcumin doses are warranted. This 12-week study was carried out to examine the effects of adjunctive curcumin for the treatment of MDD. In this double-blind, placebo-controlled trial, 65 participants with MDD were randomized to receive either adjunctive curcumin (increasing dose from 500 to 1500?mg/day) or placebo for 12?weeks. Four weeks after the active treatment phase, a follow-up visit was conducted at week 16. Assessments of the primary, i.e., the Montgomery-Asberg Depression Rating Scale (MADRS), and secondary, i.e., the Hamilton Anxiety Rating Scale (HAM-A), outcome measures were rated at baseline and 2, 4, 8, 12, and 16?weeks later. Curcumin was more efficacious than placebo in improving MADRS scores with significant differences between curcumin and placebo emerging at weeks 12 and 16. The effects of curcumin were more pronounced in males compared to females. There were no statistically significant treatment-emerging adverse effects and no significant effects of curcumin on blood chemistry and ECG measurements. Adjunctive curcumin has significant antidepressant effects in participants with MDD as evidenced by significant benefits occurring 12 and 16?weeks after treatment initiation. Curcumin administration was safe and well-tolerated even when combined with antidepressants. Future trials should include treatment-by-sex interactions to examine putative antidepressant effects of immune-modifying compounds.
机译:摘要免疫炎症和氧化 - 亚硝化(IO&NS)应激途径的活化起着重大抑郁(MDD)的作用。证据表明,姜黄素(500-1000?Mg /天),具有强抗IO&NS性质的多酚,可以具有单药治疗或作为抑郁症的辅助治疗。有必要进行延长治疗期的进一步对照试验(>?8?周)和更高的姜黄素剂量。进行了该12周的研究,以检查辅助姜黄素治疗MDD的疗效。在这种双盲,安慰剂对照试验中,65名与MDD的参与者随机分配接受辅助姜黄素(从500至1500×mg /天增加剂量)或安慰剂12?周。活动治疗阶段四周后,第16周进行了后续访问。评估初级,即蒙哥马利 - 阿伯格抑郁率(MADRS)和中学,即汉密尔顿焦虑评级规模(火腿 - a),结果措施在基线和2,4,8,12和16岁时被评定为16个星期后。姜黄素比安慰剂更有效力,改善MADRS评分,在第12周和16周内出现姜黄素和安慰剂的显着差异。与女性相比,姜黄素的作用更加明显。没有统计学上显着的治疗产生的不良影响,姜黄素对血液化学和心电图测量没有显着影响。辅助姜黄素对MDD的参与者具有显着的抗抑郁作用,如在治疗开始后发生的显着效果导致的显着效果。即使与抗抑郁药结合,姜黄素给药也是安全且耐受性。未来的试验应包括逐种治疗相互作用以检查免疫改性化合物的推定抗抑郁作用。

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