Inhibition of antigen-induced airway hyperresponsiveness in rats: effects of ozagrel (a thromboxane A2 synthase inhibitor) and of CV-3988 (a platelet activating factor antagonist).

M Misawa, Y Chiba
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Abstract

The effects of ozagrel, a thromboxane A2 (TXA2) synthase inhibitor, and CV-3988, a platelet activating factor (PAF) antagonist, was investigated on the repeatedly antigenic challenge-induced airway hyperresponsiveness (AHR) in rats. Rats were actively sensitized with DNP-Ascaris antigen and received 3 inhalations of antigen (challenges) or saline (sensitized control) every 48 hr. These animals were also pretreated with ozagrel (100 mg/kg, p.o., 30 min before), CV-3988 (3 mg/kg, i.v., 5 min before) or respective vehicle (water and saline, respectively) before each inhalation of antigen or saline. The in vivo airway responsiveness to cumulatively inhaled acetylcholine (ACh; 0.001-0.03%, each for 3 min) was measured 24 hr after the last inhalation of antigen or saline under anesthesia. A marked AHR was observed after repeated antigenic challenge when compared with the sensitized control group (5.5-9.5 times in order). This AHR was significantly, but partly, attenuated by pretreatment with ozagrel although this treatment alone had no effect on the airway responsiveness to inhaled ACh in sensitized control animals. On the other hand, CV-3988 had no inhibitory effect on this AHR. These findings suggest that TXA2, but not PAF, is one of the most important mediators participating in the pathogenesis of the antigen-induced AHR in rats.

抑制大鼠抗原诱导的气道高反应性:奥扎格雷尔(一种血栓素A2合成酶抑制剂)和CV-3988(一种血小板活化因子拮抗剂)的作用
研究了血栓素A2 (TXA2)合成酶抑制剂ozagrel和血小板活化因子(PAF)拮抗剂CV-3988对反复抗原刺激诱导大鼠气道高反应性(AHR)的影响。用dnp -蛔虫抗原主动致敏大鼠,每48小时吸入3次抗原(激发)或生理盐水(致敏对照组)。这些动物在每次吸入抗原或生理盐水之前,分别用ozagrel (100mg /kg,口服,30分钟前)、CV-3988 (3mg /kg,静脉注射,5分钟前)或各自的载体(分别为水和生理盐水)进行预处理。体内气道对累积吸入乙酰胆碱(ACh;于麻醉下最后一次吸入抗原或生理盐水24小时后测定。与致敏对照组(依次为5.5 ~ 9.5次)相比,经多次抗原激射后AHR显著。虽然在致敏的对照动物中,ozagrel预处理对吸入乙酰胆碱的气道反应性没有影响,但这种AHR明显(但部分)减弱。另一方面,CV-3988对该AHR无抑制作用。这些发现表明,TXA2是参与大鼠抗原诱导AHR发病的最重要的介质之一,而不是PAF。
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