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环氧化酶抑制剂氟比洛芬和H1组胺受体拮抗剂特非那定单独及联合应用对人变应原诱导的速发型支气管收缩的影响。

Effects of a cyclo-oxygenase inhibitor, flurbiprofen, and an H1 histamine receptor antagonist, terfenadine, alone and in combination on allergen induced immediate bronchoconstriction in man.

作者信息

Curzen N, Rafferty P, Holgate S T

机构信息

Medicine 1, Southhampton General Hospital.

出版信息

Thorax. 1987 Dec;42(12):946-52. doi: 10.1136/thx.42.12.946.

Abstract

The effect of flurbiprofen, a potent cyclo-oxygenase inhibitor, on histamine and methacholine reactivity was assessed in seven atopic subjects with asthma. Flurbiprofen 150 mg daily for three days displaced the histamine-FEV1 concentration-response curve to the right by 1.5 doubling doses, whereas no effect was observed on the response to methacholine. Subsequently the effects of flurbiprofen and terfenadine, a specific H1 histamine receptor antagonist, on allergen induced bronchoconstriction were studied in seven atopic but non-asthmatic subjects. The subjects inhaled the concentration of grass pollen allergen that had previously been shown to produce a 20% fall in FEV1 on separate occasions after prior treatment with placebo, flurbiprofen 150 mg daily for three days, terfenadine 180 mg three hours before challenge, and the combination of flurbiprofen and terfenadine. After placebo, allergen challenge caused a mean (SEM) maximum fall in FEV1 of 37.6% (2.6%) after 20 (3.7) minutes, followed by a gradual recovery to within 15% of baseline at 60 minutes. Terfenadine reduced the maximum allergen provoked fall in FEV1 to 21.5% (2.2%) and reduced the area under the time-response curve (AUC) by 50% (6%). Flurbiprofen alone reduced the mean maximum fall in FEV1 to 29.6% (3.2%) and reduced the AUC by 26%. The effect of the combination of flurbiprofen and terfenadine did not differ significantly from that of terfenadine alone. We conclude that histamine and prostaglandins contribute to immediate allergen induced bronchoconstriction and that a complex interaction occurs between the two classes of mediators.

摘要

在7名患有哮喘的特应性受试者中评估了强效环氧化酶抑制剂氟比洛芬对组胺和乙酰甲胆碱反应性的影响。每天服用150 mg氟比洛芬,持续三天,可使组胺 - FEV1浓度 - 反应曲线向右移动1.5倍剂量,而对乙酰甲胆碱的反应未观察到影响。随后,在7名特应性但非哮喘受试者中研究了氟比洛芬和特非那定(一种特异性H1组胺受体拮抗剂)对变应原诱导的支气管收缩的影响。受试者在分别接受安慰剂、每天150 mg氟比洛芬连续三天、激发前3小时服用180 mg特非那定以及氟比洛芬和特非那定联合治疗后,吸入先前已证明可使FEV1下降20%的草花粉变应原浓度。服用安慰剂后,变应原激发在20(3.7)分钟后导致FEV1平均(SEM)最大下降37.6%(2.6%),随后在60分钟时逐渐恢复至基线的15%以内。特非那定将变应原激发引起的FEV1最大下降降至21.5%(2.2%),并使时间 - 反应曲线下面积(AUC)减少50%(6%)。单独使用氟比洛芬将FEV1的平均最大下降降至29.6%(3.2%),并使AUC减少26%。氟比洛芬和特非那定联合使用的效果与单独使用特非那定的效果无显著差异。我们得出结论,组胺和前列腺素促成了变应原诱导的即刻支气管收缩,并且这两类介质之间发生了复杂的相互作用。

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