Day S M, Lockhart J C, Ferrell W R, McLean J S
Biological Sciences, University of Paisley, Paisley PA1 2BE, Scotland, UK.
Ann Rheum Dis. 2004 Dec;63(12):1564-70. doi: 10.1136/ard.2003.017269.
Nitrergic and prostanoid pathways have both been implicated in inflammatory processes.
To investigate their respective contributions in a rat model of chronic arthritis.
Male Wistar rats (n = 4-6/group) received either an intra-articular injection of 2% carrageenan/4% kaolin (C/K) or intra- and periarticular injections of Freund's complete adjuvant (FCA; 10 mg/ml M tuberculosis). Joint diameter, urinary nitric oxide metabolites (NO(x)), and prostaglandin E(2) (PGE(2)) levels were measured as indices of the inflammatory process. A prophylactic and therapeutic (day 5) dose ranging study of an inducible nitric oxide synthase inhibitor, L-N-(1-iminoethyl)-lysine (L-NIL), and a cyclo-oxygenase-2 (COX-2) inhibitor, SC-236, was performed with the drugs given subcutaneously. Submaximal doses were identified and used for combination studies. Appropriate vehicle controls were included.
L-NIL and SC-236 dose dependently inhibited C/K induced acute joint swelling, the magnitude being greatest when they were given in combination. Both prophylactic and therapeutic administration of SC-236 in the FCA induced model of chronic arthritis produced a dose dependent reduction in all the measures assessed. However, although L-NIL demonstrated similar dose dependent inhibition of urinary NO(x) and PGE(2) levels, joint swelling was significantly exacerbated in this model. Co-administration of the inhibitors nullified the benefits of SC-236.
Whereas COX-2 derived prostaglandins are proinflammatory in both acute and chronic joint inflammation, NO seems to have divergent roles, being anti-inflammatory in chronic and proinflammatory in acute joint inflammation.
一氧化氮能和前列腺素途径均与炎症过程有关。
在大鼠慢性关节炎模型中研究它们各自的作用。
雄性Wistar大鼠(每组n = 4 - 6只)接受关节内注射2%角叉菜胶/4%高岭土(C/K)或关节内及关节周围注射弗氏完全佐剂(FCA;10 mg/ml结核分枝杆菌)。测量关节直径、尿中一氧化氮代谢产物(NO(x))和前列腺素E2(PGE(2))水平作为炎症过程的指标。对诱导型一氧化氮合酶抑制剂L-N-(1-亚氨基乙基)-赖氨酸(L-NIL)和环氧化酶-2(COX-2)抑制剂SC-236进行预防性和治疗性(第5天)剂量范围研究,药物皮下注射。确定亚最大剂量并用于联合研究。纳入适当的溶媒对照。
L-NIL和SC-236剂量依赖性地抑制C/K诱导的急性关节肿胀,联合给药时抑制程度最大。在FCA诱导的慢性关节炎模型中,SC-236的预防性和治疗性给药均使所有评估指标呈剂量依赖性降低。然而,尽管L-NIL对尿中NO(x)和PGE(2)水平表现出类似的剂量依赖性抑制,但在该模型中关节肿胀明显加重。联合使用抑制剂消除了SC-236的益处。
在急性和慢性关节炎症中,COX-2衍生的前列腺素均具有促炎作用,而NO似乎具有不同作用,在慢性关节炎症中具有抗炎作用,在急性关节炎症中具有促炎作用。