Dyson M C, Bellan J A, Minkes R K, Beckerman R C, Wegmann M J, Braquet P, McNamara D B, Kadowitz P J
Department of Pharmacology, Tulane University School of Medicine, New Orleans, Louisiana.
J Pharmacol Exp Ther. 1990 Dec;255(3):1320-7.
The effects of SK&F 95587 (4[2-(benzenesulfonamido)-ethyl] phenoxyacetic acid), a thromboxane (TX) receptor blocking agent, on bronchoconstrictor responses were investigated in paralyzed, anesthetized, mechanically ventilated cats. Intravenous injections of the TXA2 receptor mimics, U-46619 [(15S)-hydroxy-11 alpha,9 alpha-(epoxymethano)prosta5Z,13E-dienoic acid] and U-44069 (9,11-dideoxy-11 alpha,9 alpha-epoxymethano PGF2 alpha), produced dose-related increases in transpulmonary pressure and lung resistance and decreases in dynamic compliance. After administration of SK&F 95587, 5 mg/kg i.v., bronchoconstrictor responses to U-46619 and U-44069 were reduced markedly, whereas airway responses to prostaglandin (PG)F2 alpha, serotonin, PGD2 or the PGD2 metabolite, 11 beta-PGF2 alpha, were not altered. The duration of action of SK&F 95587 was greater than 3 hr, and the blockade was overcome when 10-fold larger doses of the TXA2 mimics were administered. Bronchoconstrictor responses to platelet-activating factor (PAF) were blocked by SK&F 95587 and by the novel PAF receptor antagonist, BN 50730. BN 50730 also blocked the fall in systemic arterial pressure in response to PAF. However, BN 50730 did not influence airway responses to U-46619, PGF2 alpha, PGD2 or serotonin and had no effect on baseline bronchomotor tone or arterial pressure. The PAF receptor antagonism with BN 50730 was overcome when 10-fold larger doses of PAF were administered and the dose-response curves for changes in lung resistance and dynamic compliance were shifted to the right in a parallel manner. The present data suggest that SK&F 95587 has selective TX receptor blocking activity, and that BN 50730 has selective PAF receptor blocking properties in the airways of the cat. The present data also provide support for the hypothesis that bronchoconstrictor responses to PAF are mediated by specific receptors, which are coupled to a phospholipase and, when activated, result in the release of TXA2 and contraction of airway smooth muscle.
在麻痹、麻醉、机械通气的猫身上研究了血栓素(TX)受体阻断剂SK&F 95587(4-[2-(苯磺酰胺基)-乙基]苯氧基乙酸)对支气管收缩反应的影响。静脉注射TX A2受体模拟物U-46619[(15S)-羟基-11α,9α-(环氧亚甲基)前列腺素5Z,13E-二烯酸]和U-44069(9,11-二脱氧-11α,9α-环氧亚甲基前列腺素F2α),可使跨肺压和肺阻力呈剂量相关增加,动态顺应性降低。静脉注射5mg/kg的SK&F 95587后,对U-46619和U-44069的支气管收缩反应明显减弱,而对前列腺素(PG)F2α、5-羟色胺、PGD2或PGD2代谢物11β-PGF2α的气道反应未改变。SK&F 95587的作用持续时间超过3小时,当给予10倍剂量的TX A2模拟物时,阻断作用被克服。对血小板活化因子(PAF)的支气管收缩反应被SK&F 95587和新型PAF受体拮抗剂BN 50730阻断。BN 50730也可阻断因PAF引起的体循环动脉压下降。然而,BN 50730不影响对U-46619、PGF2α、PGD2或5-羟色胺的气道反应,对基线支气管运动张力或动脉压无影响。当给予10倍剂量的PAF时,BN 50730的PAF受体拮抗作用被克服,肺阻力和动态顺应性变化的剂量-反应曲线以平行方式右移。目前的数据表明,SK&F 95587具有选择性TX受体阻断活性,而BN 50730在猫气道中具有选择性PAF受体阻断特性。目前的数据也支持以下假说:对PAF的支气管收缩反应由特定受体介导,这些受体与磷脂酶偶联,激活后导致TX A2释放和气道平滑肌收缩。
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