Herbert J M, Fraisse L, Bachy A, Valette G, Savi P, Laplace M C, Lassalle J, Roche B, Lale A, Keane P E
Sanofi Recherche, Toulouse, France.
J Lipid Mediat. 1993 Aug;8(1):31-51.
SR 27388 (N-(2-dimethylaminoethyl)-N-(3-pyridinylmethyl[4-(3,5-di(tert- butyl)-4-hydroxylphenyl)thiazol-2-yl]amine) is a potent and competitive antagonist of the binding of [3H]PAF to its receptor on rabbit platelets exhibiting an equilibrium inhibition constant for PAF binding of 10.5 +/- 1.2 nM (n = 3). SR 27388 potently inhibited PAF-induced aggregation of rabbit platelets in vitro (IC50 = 65 +/- 12 nM) (n = 4). In this respect, SR 27388 was as potent as the triazolothienodiazepine WEB-2086 against PAF-induced aggregation of rabbit platelets and had no effect on the action of other platelet aggregating agents. SR 27388 prevented in a dose-dependent manner the formation of thiobarbituric acid reactive substances during membrane peroxidation (IC50 = 0.7 microM) and inhibited reduction of the stable 1,1-diphenyl-2-picrylhydrazyl radical, indicating that the antioxidant potency of SR 27388 was due to an efficient radical scavenging activity. SR 27388 displayed marked in vitro inhibition of zymosan-induced oxidative burst in human monuclear cells (IC50 = 3 microM). In vivo, SR 27388 protected mice from 100 micrograms/kg PAF-induced death with an ED50 value of 500 micrograms/kg, when given i.v., 5 min before PAF challenge or p.o. (ED50 = 800 micrograms/kg) when given 1 h before PAF administration. Similarly, i.v. or oral doses of SR 27388 afforded in mice complete protection against endotoxin-induced lethality (ED50 values were 250 micrograms/kg and 1.3 mg/kg, respectively). Neither BHT, vitamin E nor catechin exhibited significant protection against PAF- or endotoxin-induced death. In ovalbumin-presensitized rabbits, SR 27388 premixed with the allergen inhibited in a dose-dependent manner allergen-induced oedema formation in the skin (ED50 = 0.1 mumol/site). After an i.v. administration of 10 mg/kg, SR 27388 significantly protected mice against alloxan-induced diabetes. These results show that SR 27388 is a potent and orally active dual PAF receptor antagonist and antioxidant.
SR 27388(N-(2-二甲基氨基乙基)-N-(3-吡啶基甲基)[4-(3,5-二叔丁基-4-羟基苯基)噻唑-2-基]胺)是一种强效竞争性拮抗剂,可抑制[3H]血小板活化因子(PAF)与兔血小板上其受体的结合,PAF结合的平衡抑制常数为10.5±1.2 nM(n = 3)。SR 27388在体外能有效抑制PAF诱导的兔血小板聚集(IC50 = 65±12 nM)(n = 4)。在这方面,SR 27388对PAF诱导的兔血小板聚集的抑制作用与三唑并噻吩二氮䓬WEB-2086相当,且对其他血小板聚集剂的作用无影响。SR 27388能以剂量依赖方式阻止膜过氧化过程中硫代巴比妥酸反应性物质的形成(IC50 = 0.7 microM),并抑制稳定的1,1-二苯基-2-苦基肼自由基的还原,表明SR 27388的抗氧化能力归因于其高效的自由基清除活性。SR 27388在体外对酵母聚糖诱导的人单核细胞氧化爆发有显著抑制作用(IC50 = 3 microM)。在体内,当在PAF攻击前5分钟静脉注射或在PAF给药前1小时口服时,SR 27388能保护小鼠免受100微克/千克PAF诱导的死亡,ED50值分别为500微克/千克和800微克/千克。同样,静脉注射或口服SR 27388能使小鼠完全免受内毒素诱导的致死作用(ED50值分别为250微克/千克和1.3毫克/千克)。丁基羟基甲苯、维生素E和儿茶素对PAF或内毒素诱导的死亡均未表现出显著保护作用。在卵清蛋白预致敏的兔中,与变应原预混合的SR 27388能以剂量依赖方式抑制变应原诱导的皮肤水肿形成(ED50 = 0.1微摩尔/部位)。静脉注射10毫克/千克的SR 27388后,能显著保护小鼠免受四氧嘧啶诱导的糖尿病。这些结果表明,SR 27388是一种强效且口服活性的双重PAF受体拮抗剂和抗氧化剂。
Zotero 插件