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特非那定和氟比洛芬对高渗盐水诱导的支气管收缩的抑制作用。组胺起主要作用的证据。

Inhibition of hypertonic saline-induced bronchoconstriction by terfenadine and flurbiprofen. Evidence for the predominant role of histamine.

作者信息

Finnerty J P, Wilmot C, Holgate S T

机构信息

Immunopharmacology Group, Southampton General Hospital, United Kingdom.

出版信息

Am Rev Respir Dis. 1989 Sep;140(3):593-7. doi: 10.1164/ajrccm/140.3.593.

Abstract

We investigated the possible inhibitory effects of terfenadine, a histamine H1-receptor antagonist, and flurbiprofen, a cyclooxygenase inhibitor, on the bronchoconstrictor effect of inhaled 3.6% hypertonic saline in a randomized, double-blind study. Nine mildly asthmatic subjects with a history of exercise-induced asthma took part. This was conducted, first as a dose-response study and, second, as a time-course study. In the dose-response study, the provocative dose of saline-laden air causing a 25% fall in FEV1 was calculated (PD25). Terfenadine (180 mg) and the combination of terfenadine (180 mg) plus flurbiprofen (100 mg) both protected significantly against hypertonic saline challenge, achieving increases in PD25 values by factors of 7.24 and 6.30, respectively. Flurbiprofen (100 mg) also displaced the dose-response to the right, increasing the PD25 by a factor of 1.92, but this protection was significantly less than that afforded by terfenadine. In the time-course studies, a single inhalation of hypertonic saline previously shown to cause at least a 25% fall in FEV1 was administered, and FEV1, was followed for 30 min. Preadministration of terfenadine reduced the mean area under the curve of percentage fall in FEV1-time response by 68.5%, with similar results obtained with the combination of terfenadine and flurbiprofen. We conclude that the bronchoconstriction in asthma provoked by inhaled hypertonic saline is mediated predominantly through the hyperosmolar release of histamine from airway mast cells, with a minor contribution being made by prostanoids.

摘要

在一项随机、双盲研究中,我们研究了组胺H1受体拮抗剂特非那定和环氧化酶抑制剂氟比洛芬对吸入3.6%高渗盐水所致支气管收缩效应的可能抑制作用。9名有运动诱发性哮喘病史的轻度哮喘患者参与了研究。该研究首先作为剂量反应研究进行,其次作为时间进程研究进行。在剂量反应研究中,计算出使第一秒用力呼气容积(FEV1)下降25%的含盐水空气激发剂量(PD25)。特非那定(180毫克)以及特非那定(180毫克)加氟比洛芬(100毫克)的组合均对高渗盐水激发有显著保护作用,PD25值分别增加了7.24倍和6.30倍。氟比洛芬(100毫克)也使剂量反应曲线右移,PD25增加了1.92倍,但这种保护作用明显小于特非那定。在时间进程研究中,吸入一次先前已证明会使FEV1至少下降25%的高渗盐水,然后对FEV1进行30分钟的监测。预先给予特非那定可使FEV1时间反应下降百分比曲线下的平均面积减少68.5%,特非那定与氟比洛芬联合使用也得到了类似结果。我们得出结论,吸入高渗盐水诱发的哮喘中的支气管收缩主要通过气道肥大细胞组胺的高渗性释放介导,前列腺素起次要作用。

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