University of Sulaimani, College of Nursing, Department of Community Health Nursing, Sulaimani, Kurdistan Region, Iraq.
Hawler Medical University, College of Pharmacy, Department of Clinical Pharmacy, Erbil, Kurdistan Region, Iraq; Pharmacy department, School of Medicine, University of Kurdistan Hewlˆer (UKH), Erbil, Kurdistan Region, Iraq.
Brain Res Bull. 2024 Oct 1;216:111047. doi: 10.1016/j.brainresbull.2024.111047. Epub 2024 Aug 10.
Immune dysregulation can play a role in depression pathophysiology, and immunological antagonists can improve depressive symptoms in treatment-resistant bipolar depression (TRD) patients according to studies.
To evaluate the anti-depressant effects of the anti-inflammatory drug, pentoxifylline (PTX) in TRD bipolar I/II adult subjects.
This 12-week, randomized, double-blind, placebo-controlled, parallel-group trial of 60 participants was conducted at Hawler Psychiatric Hospital and Private Clinic in Erbil, Iraq. Participants were confirmed as being qualified for bipolar I/II depression based on DSM-5 criteria. Data were analyzed using modified intent-to-treat analysis.
There were no significant differences between the two groups in Hamilton Rating Scale for Depression-17 (HAM-D-17) scores (χ=1.9, P =.48) or a significant time × treatment interaction (χ=7.1, P=.54). Nevertheless, a significant effect of time was observed with both groups' reduction in HAM-D-17 scores from the start to the endpoint (χ= 2.11, P=.002). Besides, a significant time × treatment × CRP interaction was found (χ=3.1, P=0.016), where there was more reduction in HAM-D-17 score in PTX-treated subjects with CRP> 7.1 mg/L. The response rate difference between PTX and the placebo group did not reach a significance level (χ=0.84, p=0.43). Furthermore, serum concentrations of TNF-α, CRP, and IL-6 significantly reduced at week 12 in the PTX group (P=.007,.04, and <.001, respectively).
The current proof of concept study found that in terms of overall anti-depressant effectiveness in bipolar patients with TRD, PTX is not superior to placebo. However, it may improve depressive mood in a subpopulation of subjects with a higher pretreatment inflammatory profile.
免疫失调在抑郁症发病机制中起作用,根据研究,免疫抑制剂可改善治疗抵抗性双相抑郁症(TRD)患者的抑郁症状。
评估抗炎药己酮可可碱(PTX)在 TRD 双相 I/II 成年患者中的抗抑郁作用。
这是一项在伊拉克埃尔比勒 Hawler 精神病院和私人诊所进行的为期 12 周、随机、双盲、安慰剂对照、平行组试验,共纳入 60 名参与者。根据 DSM-5 标准,参与者被确认为符合双相 I/II 型抑郁症标准。采用意向治疗分析对数据进行分析。
两组间汉密尔顿抑郁量表-17 项(HAM-D-17)评分(χ=1.9,P=.48)或时间×治疗交互作用(χ=7.1,P=.54)无显著差异。然而,两组 HAM-D-17 评分均从起点降至终点(χ=2.11,P=.002),且存在显著的时间效应。此外,还发现 CRP 水平>7.1mg/L 的 PTX 治疗组 HAM-D-17 评分降低更多,存在显著的时间×治疗×CRP 交互作用(χ=3.1,P=0.016)。PTX 组与安慰剂组间的应答率差异无统计学意义(χ=0.84,p=0.43)。此外,PTX 组治疗 12 周时 TNF-α、CRP 和 IL-6 血清浓度显著降低(P=.007、.04 和 <.001)。
本概念验证研究发现,在治疗抵抗性双相患者的整体抗抑郁效果方面,PTX 并不优于安慰剂。然而,它可能会改善炎症前水平较高的患者亚群的抑郁情绪。
