Objective: To explore the effect of berberine on chronic inflammatory pain and the comorbid depression and the associated mechanisms. Methods: Forty healthy male ICR mice (2 months, 25-30 g) were used in the present study. The chronic inflammatory pain was induced by intraplantar injection of complete freund's adjuvant (CFA) to the hind paws. All animals were divided into 4 groups (n=10 for each group) according to random number table: the saline group (group A), the chronic pain group (group B), the saline+ berberine group (group C) and the chronic pain+ berberine group (group D). The baseline data of pain and depressive performance were measured on the day before any drug treatment.On d1, mice of B and D groups received intraplantar injections of 50 μl CFA emulsion (1∶1 diluted with saline); mice of A and C groups received intraplantar injections of the same volume of saline. During d15-d21, mice of C and D groups received intraperitoneal injections of berberine (50 mg/kg, daily for 7 days); mice of A and B groups received the equal volume of saline. The Hargreaves tests and the Von Frey tests were conducted before the injection of CFA and on d7, d14, d17 and d21 to measure the thermal and mechanical pain thresholds. The forced swimming tests and novelty-suppressed feeding tests were performed before the injection of CFA and on d21 to measure the depressive performance. After the behavioral tests, the levels of inflammatory cytokines interleukin-1β (IL-1β), interleukin-6 (IL-6), tumor necrosis factor-α (TNF-α) at the lumbar (L4-L5) spinal cord were examined by enzyme-linked immunosorbent assay(ELISA). The mRNA level of chemokine C-C motif ligand 2 (CCL2) in the lumbar spinal cord was examined by quantitative real-time polymerase chain reaction(qRT-PCR). Results: Compared with group A, the thermal withdrawal latency of group B mice on d7, d14, d17, d21 was declined[(3.40±0.67)s vs (10.55±1.58)s, (7.49±1.04)s vs (11.47±1.92)s, (6.46±0.56)s vs (11.60±1.86)s, (6.04±0.54)s vs (10.33±1.59)s, all P<0.01], and the mechanical threshold was also decreased[(0.15±0.03)g vs (0.78±0.24)g, (0.23±0.12)g vs (0.60±0.16)g, (0.30±0.12)g vs (0.72±0.25)g, (0.40±0.00)g vs (0.72±0.19)g, all P<0.01], on d21 the immobility time was increased[(161.60±35.79)s vs (88.92±53.24)s , P<0.05]and the time of feeding latency was decreased[(227.40±57.5)s vs (77.25±26.45)s, P<0.01], suggesting that CFA could induce hyperalgesia and depression. After berberine treatment (daily for 7 days), compared with group B, the thermal withdrawal latency of group D mice was increased[(9.99±2.68)s vs (6.04±0.54)s, P<0.01], the mechanical threshold was elevated[(0.80±0.21)g vs (0.40±0.00)g, P<0.01], the immobility time was decreased[(92.97±44.31)s vs (161.60±35.79)s, P<0.05], and the feeding latency was declined[(105.00±50.00)s vs (227.40±57.5)s, P<0.01]. Compared with group A, the concentrations of spinal IL-1β, IL-6 and TNF-α in group B were increased[(29.90±4.87)pg/ml vs (21.00±5.46)pg/ml, (131.10±26.12)pg/ml vs (60.68±23.47)pg/ml, (21.54±4.93)pg/ml vs (11.39±3.66) pg/ml , all P<0.01], the mRNA level of CCL2 was upregulated[(2.21±0.60) vs (1.00±0.37), P<0.01]. After berberine treatment (daily for 7 days), compared with group B, the concentrations of IL-1β, IL-6 and TNF-α in group D were decreased[(19.44±4.83)pg/ml vs (29.90±4.87) pg/ml , (57.82±32.28)pg/ml vs (131.10±26.12)pg/ml , (9.29±2.46)pg/ml vs (21.54±4.93) pg/ml, all P<0.01], the mRNA level of CCL2 was downregulated[(1.33±0.40)vs (2.21±0.60), P<0.05]. Conclusion: Berberine can reverse chronic inflammatory pain induced by CFA and alleviated the comorbid depression. Its anti-nociceptive and anti-depressive effects may associate with downregulation of the spinal levels of the inflammatory cytokines and mRNA transcription of CCL2.
目的: 探讨盐酸小檗碱(BBR)对小鼠慢性炎症痛及其伴发的抑郁样症状的影响及其机制。 方法: 本实验使用雄性ICR小鼠40只,2月龄,体质量25~30 g。采用小鼠足底注射完全弗氏佐剂(CFA)的方法建立慢性痛动物模型。应用随机数字表法将小鼠分为4组(n=10):生理盐水组(A组)、慢性痛组(B组)、生理盐水+BBR组(C组)、慢性痛+BBR组(D组)。所有动物在注射CFA或生理盐水之前均进行疼痛和抑郁行为学实验以测量行为学基线值。之后在实验第1天(d1),B组和D组足底注射50 μl CFA(生理盐水1∶1稀释),A组和C组足底注射等量生理盐水;在d15~d21,C组和D组腹腔注射BBR 50 mg/kg,共持续7 d,A组和B组注射等容量生理盐水。通过Hargreaves方法和Von Frey纤毛在建模以前、d7、d14、d17和d21分别进行热痛和机械痛阈值测定;通过强迫游泳和摄食抑制实验在建模以前和d21进行抑郁样行为指标测定。在行为学结束之后处死所有动物,取L4~L5段脊髓采用酶联免疫吸附试验(ELISA)检测各组小鼠脊髓中白细胞介素1β(IL-1β)、白细胞介素6(IL-6)和肿瘤坏死因子α(TNF-α)的水平,并通过实时定量聚合酶链反应(qRT-PCR)分析CC趋化因子配体2(CCL2)的mRNA水平。 结果: 与A组相比,B组小鼠在d7、d14、d17、d21的热痛阈值均显著降低[(3.40±0.67)s比(10.55±1.58)s、(7.49±1.04)s比(11.47±1.92)s、(6.46±0.56)s比(11.60±1.86)s、(6.04±0.54)s比(10.33±1.59)s,均P<0.01],机械痛阈值均显著降低[(0.15±0.03)g比(0.78±0.24)g、(0.23±0.12)g比(0.60±0.16)g、(0.30±0.12)g比(0.72±0.25)g、(0.40±0.00)g比(0.72±0.19)g,均P<0.01],在d21强迫游泳不动时间延长[(161.60±35.79)s比(88.92±53.24)s,P<0.05],摄食潜伏期延长[(227.40±57.5)s比(77.25±26.45)s,P<0.01],提示CFA可诱发痛觉过敏和抑郁样行为。连续7 d BBR处理后,与B组比较,D组小鼠的热痛阈值[(9.99±2.68)s比(6.04±0.54)s,P<0.01]显著升高,机械痛阈值显著升高[(0.80±0.21)g比(0.40±0.00)g,P<0.01],其不动时间缩短[(92.97±44.31)s比(161.60±35.79)s,P<0.05]以及摄食潜伏期缩短[(105.00±50.00)s比(227.40±57.5)s,P<0.01]。炎症因子和趋化因子水平检测提示,与A组比较,B组小鼠脊髓中IL-1β、IL-6和TNF-α的浓度均升高[(29.90±4.87)pg/ml比(21.00±5.46)pg/ml、(131.10±26.12)pg/ml比(60.68±23.47)pg/ml、(21.54±4.93)pg/ml比(11.39±3.66) pg/ml,均P<0.01],CCL2的mRNA表达也显著上调[(2.21±0.60)比(1.00±0.37) ,P<0.01]。连续7 d BBR处理后,与B组比较,D组小鼠脊髓IL-1β、IL-6和TNF-α的浓度显著下调[(19.44±4.83)pg/ml比(29.90±4.87)pg/ml、(57.82±32.28)pg/ml比(131.10±26.12) pg/ml、(9.29±2.46) pg/ml比(21.54±4.93) pg/ml,均P<0.01],CCL2的mRNA水平显著降低[(1.33±0.40 )比(2.21±0.60),P<0.05]。 结论: 盐酸小檗碱可以改善CFA诱导的慢性炎症痛以及与其共患的抑郁样行为,其机制可能与盐酸小檗碱抑制炎症因子释放和下调CCL2的转录水平有关。.
Keywords: Depression; Inflammation; Pain; Treatment outcome.