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在大鼠急性炎症的皮下海绵植入模型中,白细胞募集并非由白三烯B1介导。

Leukocyte recruitment in the subcutaneous sponge implant model of acute inflammation in the rat is not mediated by leukotriene B1.

作者信息

Foster S J, McCormick M E, Howarth A, Aked D

出版信息

Biochem Pharmacol. 1986 May 15;35(10):1709-17. doi: 10.1016/0006-2952(86)90328-x.

Abstract

The subcutaneous sponge implant model of acute inflammation in the rat has been evaluated as a suitable test system for evaluating the potential anti-inflammatory efficacy of 5-lipoxygenase inhibitors. The inflammatory parameters measured were exudate volume and leukocyte recruitment. Specific radioimmunoassays were used to measure (1) 5-lipoxygenase (LPO) and cyclo-oxygenase (CO) activity in exudate leukocytes stimulated ex vivo with A23187, and (2) the LTB4 and PGE2 content of inflammatory exudate. The NSAIDs flurbiprofen and indomethacin inhibited cell recruitment, exudate volume and CO activity with ED50S of approximately 1 mg per kg p.o. but failed to inhibit LPO activity at 10 mg per kg p.o. Nafazatrom (Bayer 6575), quercetin and NDGA, which inhibit LPO activity in vitro, were inactive against all parameters when dosed at 100 mg per kg p.o. The "mixed inhibitors" BW755C and phenidone were approximately equipotent inhibitors of LPO activity but BW755C was 10 times more potent than phenidone against CO activity. BW755C was also greater than 10 times more potent at inhibiting cell recruitment and exudate volume than phenidone suggesting that the anti-inflammatory efficacy of the mixed inhibitors reflect their potency against CO rather than LPO activity. Time course studies demonstrated that the inhibitor effects of BW755C and phenidone on leukocyte recruitment reflected a reduction in the PGE2 but not the LTB4 content of the inflammatory exudate. Polyester sponges soaked in high concentrations of LTB4 caused only a modest (2-fold) increase in leukocyte recruitment whilst physiological levels were inactive. The results taken together suggest that CO products make a major contribution to leukocyte recruitment in this model whilst the LPO product LTB4 has little role. This model therefore is of little value for evaluating the anti-inflammatory efficacy of 5-lipoxygenase inhibitors. Moreover, the rat would appear to be unsuitable for evaluating the role of LTB4 in acute inflammation.

摘要

大鼠皮下海绵植入急性炎症模型已被评估为一种合适的测试系统,用于评估5-脂氧合酶抑制剂的潜在抗炎功效。所测量的炎症参数为渗出液体积和白细胞募集。使用特异性放射免疫分析法来测量:(1)用A23187体外刺激渗出液白细胞中的5-脂氧合酶(LPO)和环氧化酶(CO)活性;(2)炎症渗出液中白三烯B4(LTB4)和前列腺素E2(PGE2)的含量。非甾体抗炎药氟比洛芬和吲哚美辛抑制细胞募集、渗出液体积和CO活性,口服给药的半数有效剂量(ED50)约为每千克1毫克,但口服给药每千克10毫克时未能抑制LPO活性。在体外抑制LPO活性的萘扎替丁(拜耳6575)、槲皮素和去甲二氢愈创木酸,口服给药每千克100毫克时对所有参数均无活性。“混合抑制剂”BW755C和非那宗是LPO活性的近似等效抑制剂,但BW755C对CO活性的效力是非那宗的10倍。BW755C在抑制细胞募集和渗出液体积方面的效力也比非那宗强10倍以上,这表明混合抑制剂的抗炎功效反映了它们对CO而非LPO活性的效力。时间进程研究表明,BW755C和非那宗对白细胞募集的抑制作用反映了炎症渗出液中PGE2含量的降低,而非LTB4含量的降低。浸泡在高浓度LTB4中的聚酯海绵仅使白细胞募集适度增加(2倍),而生理水平则无活性。综合这些结果表明,在该模型中CO产物对白细胞募集起主要作用,而LPO产物LTB4作用很小。因此,该模型对于评估5-脂氧合酶抑制剂的抗炎功效价值不大。此外,大鼠似乎不适合用于评估LTB4在急性炎症中的作用。

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