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吸入速尿对特应性患者抗原早期反应及随后气道反应性变化的影响。

Effect of inhaled frusemide on the early response to antigen and subsequent change in airway reactivity in atopic patients.

作者信息

Verdiani P, Di Carlo S, Baronti A, Bianco S

机构信息

Department of Pneumology, G A Pizzetti Hospital, Grosseto, Italy.

出版信息

Thorax. 1990 May;45(5):377-81. doi: 10.1136/thx.45.5.377.

Abstract

The purpose of this study was to investigate whether inhaled frusemide was able to inhibit the increase in nonspecific bronchial reactivity that occurs after the early response to allergen exposure in subjects with allergic rhinitis or asthma (or both). Ten symptom free patients initially underwent a challenge with methacholine, to determine the dose of methacholine that caused a 15% fall in FEV1 (PD15 FEV1 meth) and a challenge with a specific allergen, to determine the concentration of allergen that caused a fall in FEV1 of at least 15%. On two further occasions they inhaled allergen concentration that had caused the greater than or equal to 15% fall in FEV1 preceded by inhaled frusemide (40 mg frusemide in 4 ml buffered saline) or placebo (4 ml of diluent solution), according to a randomised, double blind, crossover design. All allergen studies were separated by at least seven days. A methacholine challenge was performed two hours after the allergen challenge, a time when the early response to allergen had completely resolved. Frusemide inhibited the early response to antigen, causing mean (95% confidence interval) protection of 87.6% (96-80%) for the maximum fall in FEV1. The increase in non-specific airway reactivity that occurred after antigen when this was preceded by placebo was reduced by frusemide. The mean (95% CI) difference in PD15 values between the placebo and the frusemide days was 1.73 (2.30-1.16) doubling doses of methacholine. These results confirm that frusemide is highly effective in preventing the early response to allergen, and show that it inhibits the increase in reactivity to methacholine that follows the early response.

摘要

本研究的目的是调查吸入速尿是否能够抑制变应性鼻炎或哮喘(或两者兼具)患者在过敏原暴露早期反应后出现的非特异性支气管反应性增加。10名无症状患者最初接受了乙酰甲胆碱激发试验,以确定导致第一秒用力呼气容积(FEV1)下降15%的乙酰甲胆碱剂量(PD15 FEV1 meth),并进行了特异性过敏原激发试验,以确定导致FEV1下降至少15%的过敏原浓度。在另外两次试验中,他们按照随机、双盲、交叉设计,在吸入过敏原浓度(该浓度导致FEV1下降大于或等于15%)之前,先吸入速尿(40mg速尿溶于4ml缓冲盐水中)或安慰剂(4ml稀释液)。所有过敏原研究之间至少间隔7天。在过敏原激发试验两小时后进行乙酰甲胆碱激发试验,此时过敏原的早期反应已完全消退。速尿抑制了对抗原的早期反应,对FEV1的最大下降幅度产生了平均(95%置信区间)87.6%(96-80%)的保护作用。在安慰剂预处理后抗原激发后出现的非特异性气道反应性增加被速尿降低。安慰剂日和速尿日之间PD15值的平均(95%CI)差异为1.73(2.30-1.16)倍乙酰甲胆碱剂量。这些结果证实速尿在预防过敏原早期反应方面非常有效,并表明它抑制了早期反应后对乙酰甲胆碱反应性的增加。

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