缓激肽B1受体在慢性抗原诱导性关节炎关节内血浆外渗维持中的作用
The role of bradykinin B1 receptors in the maintenance of intra-articular plasma extravasation in chronic antigen-induced arthritis.
作者信息
Cruwys S C, Garrett N E, Perkins M N, Blake D R, Kidd B L
机构信息
Inflammation Group, London Hospital Medical College.
出版信息
Br J Pharmacol. 1994 Nov;113(3):940-4. doi: 10.1111/j.1476-5381.1994.tb17083.x.
Abstract
- The role of bradykinin B1 and B2 receptors in bradykinin- and des-Arg9-bradykinin-induced plasma extravasation in normal and inflamed rat knee joints was investigated by use of an antigen-induced model of chronic arthritis. A modification of an Evans blue extraction technique allowed the unstimulated (basal) plasma extravasation to be assessed in this model. The contributions of bradykinin B1 and B2 receptors towards basal synovial plasma extravasation were determined. 2. In normal knees, intra-articular injection of bradykinin (BK) induced plasma extravasation in a potent, dose-dependent manner with a threshold of 0.01 nmol and an ED50 of 0.1 nmol. In day 5 arthritic knees, basal plasma extravasation was substantially enhanced. Lower doses of BK had no demonstrable effect and increases above basal extravasation were first observed at 0.1 nmol. Thereafter the dose-response mirrored the response in normal knees and the maximal response was unaltered. 3. The B1 agonist, des-Arg9-BK, induced slight but significant plasma extravasation in normal knees but was less potent than bradykinin. This response was inhibited by the B1 receptor antagonist, des-Arg9, [Leu8]-BK. Lower doses of des-Arg9-BK bradykinin did not significantly increase basal extravasation in day 5 arthritic knees but, in contrast to BK, the maximal response was significantly enhanced. 4. The B2 antagonist, Hoe 140, inhibited BK-induced plasma extravasation in normal joints over a dose-range of 0.1-1.0 nmol but was relatively inactive in day 5 inflamed knees. The B1 receptor antagonist, des-Arg9, [Leu8]-BK, was relatively inactive in normal joints but showed increased potency against BK-induced plasma extravasation in day 5 arthritic joints.5. Hoe 140 and des-Arg9,[Leu8]-BK both inhibited basal extravasation in arthritic joints on days 1 and 5 post-challenge in a dose-dependent fashion. Whilst Hoe 140 was the more potent inhibitor on day 1, it was less potent than des-Arg9,[Leu8]-BK on day 5.6. Although the majority of responses to BK in normal tissue are mediated via B2 receptors, a small population of B1 receptors may exist in normal joint tissues. The data presented in this study suggest an evolving role for B1 receptors in the mediation of plasma extravasation in inflamed joint tissues. A role for BK antagonists in the treatment of arthritis is also suggested.
摘要
- 利用抗原诱导的慢性关节炎模型,研究了缓激肽B1和B2受体在缓激肽及去-Arg9-缓激肽诱导的正常和炎症大鼠膝关节血浆外渗中的作用。对伊文思蓝提取技术的改良使得在此模型中能够评估未刺激(基础)的血浆外渗情况。确定了缓激肽B1和B2受体对基础滑膜血浆外渗的贡献。2. 在正常膝关节中,关节腔内注射缓激肽(BK)以有效、剂量依赖性方式诱导血浆外渗,阈值为0.01 nmol,半数有效剂量(ED50)为0.1 nmol。在第5天的关节炎膝关节中,基础血浆外渗显著增强。较低剂量的BK无明显作用,在0.1 nmol时首次观察到高于基础外渗的增加。此后剂量反应与正常膝关节中的反应相似,最大反应未改变。3. B1激动剂去-Arg9-BK在正常膝关节中诱导轻微但显著的血浆外渗,但效力低于缓激肽。该反应被B1受体拮抗剂去-Arg9,[Leu8]-BK抑制。较低剂量的去-Arg9-BK缓激肽在第5天的关节炎膝关节中未显著增加基础外渗,但与BK相反最大反应显著增强。4. B2拮抗剂Hoe 140在0.1 - 1.0 nmol剂量范围内抑制正常关节中BK诱导的血浆外渗,但在第5天的炎症膝关节中相对无活性。B1受体拮抗剂去-Arg9,[Leu8]-BK在正常关节中相对无活性,但在第5天的关节炎关节中对BK诱导的血浆外渗显示出增强的效力。5. Hoe 140和去-Arg9,[Leu8]-BK在攻击后第1天和第5天均以剂量依赖性方式抑制关节炎关节中的基础外渗。虽然Hoe 140在第1天是更有效的抑制剂,但在第5天其效力低于去-Arg9,[Leu8]-BK。6. 尽管在正常组织中对BK的大多数反应是通过B2受体介导的,但正常关节组织中可能存在少量B1受体。本研究中呈现的数据表明B1受体在炎症关节组织血浆外渗介导中作用不断演变。还提示了BK拮抗剂在关节炎治疗中的作用。
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