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某些抗风湿药物对人多形核白细胞趋化性体外模型的影响。

The effects of some antirheumatic drugs on an in vitro model of human polymorphonuclear leucocyte chemokinesis.

作者信息

Smith M J, Walker J R

出版信息

Br J Pharmacol. 1980 Jul;69(3):473-8. doi: 10.1111/j.1476-5381.1980.tb07037.x.

Abstract

1 A rapid, reproducible in vitro assay for studying the chemokinetic movement of human polymorphonuclear leucocytes (PMNs) is described. Two synthetic peptides, formyl methionyl-leucyl-phenylalanine (FMLP) and formyl methionyl-phenylalanine (FMP), were used as a standard chemokinesins. 2 Maximal chemokinetic movement was observed with peptide concentrations of 2.5 nM (FMLP) and 100 muM (FMP). EC50 values of 650.0 +/- 60.0 pM and 27.0 +/- 3.5 muM respectively are similar to those reported for chemotactic activity of the peptides in micropore filter assays. 3 The PMN chemokinetic response to FMLP was enhanced by histamine (100 nM) and vitamin C (2.5 muM). 4 Human serum albumin was shown to induce chemokinesis but to antagonize the response to FMLP in a dose-related fashion. Fibrinogen similarly antagonized the cell response to peptide. 5 Levamisole (250 nM to 2.5 muM) significantly potentiated the chemokinetic responses to FMLP and FMP in a dose-related manner. The chemokinetic response to FMLP was unaffected by D-penicillamine (250 muM to 10 mM) while alclofenac (500 muM to 1 mM), salicylic acid (250 muM to 10 mM) and indomethacin (100 muM to 1 mM) caused dose-related inhibition.

摘要

1 描述了一种用于研究人多形核白细胞(PMN)化学动力学运动的快速、可重复的体外测定法。两种合成肽,甲酰甲硫氨酰-亮氨酰-苯丙氨酸(FMLP)和甲酰甲硫氨酰-苯丙氨酸(FMP),被用作标准趋化因子。2 在肽浓度为2.5 nM(FMLP)和100 μM(FMP)时观察到最大化学动力学运动。EC50值分别为650.0±60.0 pM和27.0±3.5 μM,与微孔滤膜测定法中报道的肽趋化活性值相似。3 组胺(100 nM)和维生素C(2.5 μM)增强了PMN对FMLP的化学动力学反应。4 人血清白蛋白被证明可诱导化学动力学,但以剂量相关方式拮抗对FMLP的反应。纤维蛋白原同样拮抗细胞对肽的反应。5 左旋咪唑(250 nM至2.5 μM)以剂量相关方式显著增强了对FMLP和FMP的化学动力学反应。对FMLP的化学动力学反应不受D-青霉胺(250 μM至10 mM)影响,而双氯芬酸(500 μM至1 mM)、水杨酸(250 μM至10 mM)和吲哚美辛(100 μM至1 mM)引起剂量相关的抑制。

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