Casals-Stenzel J
Immunopharmacology. 1987 Apr;13(2):117-24. doi: 10.1016/0162-3109(87)90048-8.
WEB 2086, a novel specific platelet activating factor (PAF) antagonist derived from triazolodiazepines, inhibited in a dose-related manner the PAF-dependent component of anaphylaxis as well as PAF-induced effects in mice and guinea pigs. In mice a lethal anaphylactic shock and a PAF-induced (100 micrograms/kg i.v.) death was inhibited by i.v. WEB 2086. The ED50 values were 13.6 and 0.37 mg/kg i.v., respectively. In actively sensitized guinea pigs, the anaphylactic lung reaction (bronchoconstriction), but not the corresponding hypotension, was prevented by oral (0.05-0.5 mg/kg) doses of WEB 2086. In contrast, in passively sensitized animals a dose-dependent inhibition of the pulmonary (bronchoconstriction) and blood pressure (hypotension) reaction due to anaphylaxis was achieved by i.v. WEB 2086. Similarly, oral (0.05-0.5 mg/kg) and i.v. (0.005-0.05 mg/kg) WEB 2086 inhibited PAF-induced reduction in respiratory flow (bronchoconstriction) and hypotension in guinea pigs. The ED50 values were 0.070 and 0.066 mg/kg p.o., and 0.017 and 0.015 mg/kg i.v., respectively. In conclusion, PAF seems to play a more major role in passive than in active anaphylaxis in guinea pigs. These results provide further evidence for an important role of PAF in anaphylaxis and support the hypothesis that PAF is involved in asthma and other allergic diseases.
WEB 2086是一种源自三唑二氮卓类的新型特异性血小板激活因子(PAF)拮抗剂,它以剂量相关的方式抑制过敏反应中PAF依赖性成分以及PAF在小鼠和豚鼠中诱导的效应。在小鼠中,静脉注射WEB 2086可抑制致死性过敏休克以及PAF诱导(静脉注射100微克/千克)的死亡。半数有效剂量(ED50)值分别为静脉注射13.6毫克/千克和0.37毫克/千克。在主动致敏的豚鼠中,口服(0.05 - 0.5毫克/千克)剂量的WEB 2086可预防过敏性肺反应(支气管收缩),但不能预防相应的低血压。相反,在被动致敏的动物中,静脉注射WEB 2086可实现对过敏性肺(支气管收缩)和血压(低血压)反应的剂量依赖性抑制。同样,口服(0.05 - 0.5毫克/千克)和静脉注射(0.005 - 0.05毫克/千克)的WEB 2086可抑制PAF诱导的豚鼠呼吸流量降低(支气管收缩)和低血压。ED50值分别为口服0.070毫克/千克和0.066毫克/千克,静脉注射0.017毫克/千克和0.015毫克/千克。总之,在豚鼠中,PAF在被动过敏反应中似乎比在主动过敏反应中发挥更主要的作用。这些结果为PAF在过敏反应中的重要作用提供了进一步的证据,并支持PAF参与哮喘和其他过敏性疾病的假说。
