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首页> 外文期刊>Life sciences >ANTI-INFLAMMATORY EFFECTS OF KAPPA-OPIOIDS IN ADJUVANT ARTHRITIS
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ANTI-INFLAMMATORY EFFECTS OF KAPPA-OPIOIDS IN ADJUVANT ARTHRITIS

机译:κ型阿片类药物在辅助性关节炎中的抗炎作用

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Current therapies for arthritis are unsatisfactory and cause serious side effects and morbidity. It has been postulated that opioid drugs may block inflammatory mediators and attenuate the joint damage in adjuvant arthritis. However, the importance of opioid receptor subtypes involved in inflammation remains to be determined because data are conflicting in this regard. The present investigation was designed to test the effects of both a kappa-agonist, (+/-)U50488H and a kappa-antagonist, MR2266 on the progression of experimental arthritis. To produce adjuvant arthritis, male Lewis rats were innoculated subcutaneously (s.c.) with 0.05 ml of Freund's complete adjuvant (10 mg/ml) into the right hind paw. The kappa-opioid agonist, (+/-)U50488H (20 mg/kg/d s.c.) and the kappa-opioid antagonist, MR2266 (20 mg/kg/d s.c.) were administered for 3 days during the primary inflammatory phase of adjuvant arthritis. There were four treatment groups; group I were non-arthritic controls and received paraffin oil vehicle and opioid injections; group II were arthritic controls and received adjuvant and saline injections; group III received adjuvant and agonist and group IV received adjuvant and antagonist. The progression of adjuvant arthritis from day 0 to 24 was monitored by body weight change, hind limb size (ipsilateral and contralateral) and a total severity score for each clinical observation of gait, coat and limb condition. On day 24 histology and radiography of the contralateral limb was performed. There was less soft-tissue swelling, as judged by time-averaged % change in the volume of the contralateral limb, in both agonist (mean +/- se: 82 +/- 5) and antagonist (77 +/- 4) treated rats compared to untreated arthritic controls (99 +/- 5, p<0.05). Other clinical measures of severity were not different between untreated and opioid-treated arthritic rats. However, the joint damage as judged by radiography was lower in kappa agonist treated rats (2.6 +/- 0.5, p<0.05) compared to untreated controls (4.1 +/- 0.5) and antagonist treatment (4.4 +/- 0.5). Microscopic pathological scores were also significantly lower in agonist (2.8 +/- 0.3, p<0.05) compared to both antagonist treated rats (4.2 +/- 0.1) and vehicle-treated controls (3.6 +/- 0.2). The results of this study show that kappa-opioid receptor agonists but not antagonists attenuate the progression of experimental arthritis. These observations have important implications for the evaluation and use of kappa-opioid agents in the management of arthritis. [References: 34]
机译:当前用于关节炎的疗法并不令人满意,并且引起严重的副作用和发病率。据推测,阿片类药物可能会阻断炎性介质并减轻佐剂性关节炎中的关节损伤。但是,与炎症相关的阿片受体亚型的重要性尚待确定,因为这方面的数据存在冲突。本研究旨在测试(+/-)U50488Hκ激动剂和MR2266κ拮抗剂对实验性关节炎进展的影响。为了产生佐剂性关节炎,将雄性Lewis大鼠皮下(s.c.)皮下接种0.05ml弗氏完全佐剂(10mg / ml)到右后爪中。在佐剂的初级炎症阶段,将κ阿片激动剂(+/-)U50488H(20 mg / kg / d sc)和κ阿片拮抗剂MR2266(20 mg / kg / d sc)给药3天关节炎。有四个治疗组。第一组为非关节炎对照组,接受石蜡油媒介物和阿片类药物注射。第二组为关节炎对照组,接受佐剂和生理盐水注射。第三组接受佐剂和激动剂,第四组接受佐剂和拮抗剂。通过体重变化,后肢大小(同侧和对侧)以及每次步态,外套和肢体状况的临床严重程度总评分来监测辅助关节炎从第0天到第24天的进展。在第24天,对侧肢进行了组织学和放射照相。根据激动剂(平均+/- se:82 +/- 5)和拮抗剂(77 +/- 4),对侧肢体的时间平均百分比变化判断,软组织肿胀较少与未治疗的关节炎对照组相比(99 +/- 5,p <0.05)。其他严重程度的临床指标在未经治疗和经阿片类药物治疗的关节炎大鼠之间没有差异。然而,与未治疗的对照组(4.1 +/- 0.5)和拮抗剂治疗(4.4 +/- 0.5)相比,用放射线照相法判断的经κ激动剂处理的大鼠(2.6 +/- 0.5,p <0.05)的关节损伤较低。与拮抗剂治疗的大鼠(4.2 +/- 0.1)和媒介物治疗的对照(3.6 +/- 0.2)相比,激动剂的微观病理学评分也显着降低(2.8 +/- 0.3,p <0.05)。这项研究的结果表明,κ阿片受体激动剂而非拮抗剂减弱了实验性关节炎的进展。这些观察结果对关节炎治疗中κ阿片类药物的评估和使用具有重要意义。 [参考:34]

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