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一氧化氮-萘普生调节大鼠弗氏佐剂性关节炎中的炎症、痛觉,并下调T细胞反应。

NO-naproxen modulates inflammation, nociception and downregulates T cell response in rat Freund's adjuvant arthritis.

作者信息

Cicala C, Ianaro A, Fiorucci S, Calignano A, Bucci M, Gerli R, Santucci L, Wallace J L, Cirino G

机构信息

Dipartimento di Farmacologia Sperimentale, Università degli Studi di Napoli - Federico II, Napoli, Italy.

出版信息

Br J Pharmacol. 2000 Jul;130(6):1399-405. doi: 10.1038/sj.bjp.0703449.

Abstract
  1. Anti-inflammatory non steroidal drugs releasing NO (NO-NSAIDs) are a new class of anti-inflammatory drugs to which has been added an NO-releasing moiety. These compounds have been shown to retain the anti-inflammatory, analgesic and antipyretic activity of the parent compound but to be devoid of gastrointestinal (GI) toxicity. 2. Freund's adjuvant (FA) arthritis was induced in rats by a single intraplantar injection into the right hindpaw of 100 microl of mycobacterium butirricum (6 mg ml(-1)). The effect of equimolar doses of naproxen (1, 3 and 10 mg kg(-1)) and NO-naproxen (1.5, 4.5 and 16 mg kg(-1)) was evaluated using two dosage regimen protocols: (i) preventive, starting oral administration of the drugs at the time of induction of arthritis and for the following 21 days (day 1 - 21); (ii) therapeutic, starting oral administration of the drugs 7 days after adjuvant injection and for the following 14 days (day 7 - 21). 3. Hindpaw swelling (days 3, 7, 11, 14, 17, 21) and nociception (days 15 and 21) were measured. On day 22 rats were sacrificed, draining lymph nodes were removed and T cells isolated. In vitro proliferation of T cells following stimulation with concanavalin A (0.5 - 5 microg ml(-1)) was measured using a tritiated thymidine incorporation assay. IL-2 receptor expression on T cells was measured by FACS analysis. 4. Naproxen and NO-naproxen showed similar activity in reducing oedema formation in the non-injected (controlateral) hindpaw. Both drugs showed anti-nociceptive effect. NO-naproxen was anti-nociceptive at a dose of 4.5 mg kg(-1) while naproxen showed the same extent of inhibition only at a dose of 10 mg kg(-1). 5. T cells were isolated and characterized by FACS analysis. Stimulation of isolated T cells with concanavallin A in vitro caused a significant increase in thymidine uptake. NO-naproxen at a dose of 4.5 mg kg(-1) inhibited T cell proliferation to the same extent as 10 mg kg(-1) of naproxen. 6. Inhibition of T cell proliferation was well correlated with reduced IL-2 receptor expression on T cells. In addition, NO-naproxen reduced both IL-1beta and TNFalpha plasma levels whilst naproxen reduced IL-1beta levels only. 7. In conclusion, both naproxen and NO-naproxen reduce inflammation and nociception associated with arthritis. In addition NO-naproxen interferes to a larger extent with cellular mechanism involved in T cell activation in rat adjuvant arthritis indicating that introduction of the NO moiety in the naproxen structure increases the effect at the level of the immune system.
摘要
  1. 释放一氧化氮的抗炎非甾体类药物(NO-NSAIDs)是一类新型抗炎药物,其结构中添加了一个能释放NO的部分。这些化合物已被证明保留了母体化合物的抗炎、镇痛和解热活性,但没有胃肠道(GI)毒性。2. 通过在大鼠右后爪足底单次注射100微升丁酸分枝杆菌(6毫克/毫升)诱导弗氏佐剂(FA)性关节炎。使用两种给药方案评估等摩尔剂量的萘普生(1、3和10毫克/千克)和NO-萘普生(1.5、4.5和16毫克/千克)的效果:(i)预防性给药,在关节炎诱导时开始口服给药,并持续21天(第1天至21天);(ii)治疗性给药,在佐剂注射7天后开始口服给药,并持续14天(第7天至21天)。3. 测量后爪肿胀(第3、7、11、14、17、21天)和痛觉(第15和21天)。在第22天处死大鼠,取出引流淋巴结并分离T细胞。使用氚化胸腺嘧啶掺入法测量用刀豆球蛋白A(0.5 - 5微克/毫升)刺激后T细胞的体外增殖。通过流式细胞术分析测量T细胞上IL-2受体的表达。4. 萘普生和NO-萘普生在减轻未注射(对侧)后爪水肿形成方面表现出相似的活性。两种药物均显示出抗伤害感受作用。NO-萘普生在剂量为4.5毫克/千克时具有抗伤害感受作用,而萘普生仅在剂量为10毫克/千克时表现出相同程度的抑制作用。5. 通过流式细胞术分析分离并鉴定T细胞。体外用刀豆球蛋白A刺激分离的T细胞导致胸腺嘧啶摄取显著增加。剂量为4.5毫克/千克的NO-萘普生抑制T细胞增殖的程度与10毫克/千克的萘普生相同。6. T细胞增殖的抑制与T细胞上IL-2受体表达的降低密切相关。此外,NO-萘普生降低了IL-1β和TNFα的血浆水平,而萘普生仅降低了IL-1β水平。7. 总之,萘普生和NO-萘普生均能减轻与关节炎相关的炎症和痛觉。此外,NO-萘普生在大鼠佐剂性关节炎中对参与T细胞活化的细胞机制有更大程度的干扰,这表明在萘普生结构中引入NO部分可增强在免疫系统水平的作用。

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