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β2 激动剂停用后不久出现的支气管反应性增加或第一秒用力呼气容积(FEV1)增加,是否反映了过敏性哮喘患者疾病的真正恶化?短效与长效β2 激动剂的比较。

Is the increase in bronchial responsiveness or FEV1 shortly after cessation of beta2-agonists reflecting a real deterioration of the disease in allergic asthmatic patients? A comparison between short-acting and long-acting beta2-agonists.

作者信息

van Schayck C P, Cloosterman S G M, Bijl-Hofland I D, van den Hoogen H, Folgering H Th M, van Weel C

机构信息

Department of General Practice, University of Nijmegen, The Netherlands.

出版信息

Respir Med. 2002 Mar;96(3):155-62. doi: 10.1053/rmed.2001.1243.

Abstract

Regular use of beta2-agonists might result in increased bronchial hyper-responsiveness (BHR) and decreased forced expiratory volume in 1 sec (FEV1). It has been suggested that these possible detrimental effects are not a real deterioration of the disease, but that it might be only a transient (rebound) effect shortly after discontinuing this regular use. Moreover, these effects are thought to occur especially during short-acting and not during long-acting beta2-agonists use. The aim of this study was to invest gate whether a rebound effect (a pharmacological deterioration effect diminishing after several hours) in FEV1 and PC20 (concentration of histamine causing a 20% fall in FEV1 with regard to baseline) occurred after cessation of regular use of beta2-agonists, and whether this occurred both after short-acting and long-acting beta2-agonists. Allergic asthmatic patients (n = 134) were randomly allocated to the use of a short-acting (salbutamol), a long-acting beta2-agonist (formoterol) or placebo for 12 weeks (double-blind, double-dummy). No other asthma medication was allowed, including inhaled corticosteroids. At the start and every 4 weeks later FEV and PC20 were measured, each time at least 12 h after the last doses of study medication, which is in the possible rebound period. To investigate whether a (transient) rebound effect occurred, parameters were additionally measured at least 72 h later after discontinuation of the study medication. After 12 weeks of short-acting beta2-agonist use, a drop was seen in FEV1 from 85.6 (+/- 2.21)% predicted to 78.8 (+/- 2.9)% predicted, measured 15 h (median) after the last doses of medication. This was significantly different compared to placebo. When measured 168 h (median) later FEV1 recovered to 85.5 (+/- 2.4)% predicted, comparable to baseline. PC20 decreased with -1.17 (+/- 0.44) doubling dose after 12 weeks of short-acting beta2-agonist use, measured 15 h after the last doses of medication, which was significantly different compared to placebo. However, 168 h later PC20 recovered slightly with +0.55 (+/- 0.34) doubling dose, but this value was still lower compared to placebo. In contrast, during long-acting beta2-agonist and placebo use no significant changes were seen. In conclusion, the use of short-acting beta2-agonists resulted in a transient (rebound) effect in FEV while the effects on PC20 may point to a real deterioration of the disease. Long-acting beta2-agonist and placebo use showed no changes. We conclude that a mono-therapy of short-acting and not of long-acting beta2-agonists might have deleterious effects in asthma.

摘要

长期使用β2激动剂可能会导致支气管高反应性(BHR)增加以及一秒用力呼气容积(FEV1)降低。有人提出,这些可能的有害影响并非疾病的真正恶化,而可能只是在停止这种长期使用后不久出现的短暂(反弹)效应。此外,这些效应被认为尤其在使用短效β2激动剂期间出现,而在使用长效β2激动剂期间不会出现。本研究的目的是调查在停止长期使用β2激动剂后,FEV1和PC20(使FEV1相对于基线下降20%的组胺浓度)是否会出现反弹效应(一种数小时后逐渐减弱的药理恶化效应),以及这种效应在短效和长效β2激动剂使用后是否都会出现。将134例过敏性哮喘患者随机分配为使用短效(沙丁胺醇)、长效β2激动剂(福莫特罗)或安慰剂,为期12周(双盲、双模拟)。不允许使用其他哮喘药物,包括吸入性糖皮质激素。在开始时以及之后每4周,测量FEV和PC20,每次均在最后一剂研究药物给药至少12小时后进行测量,此时处于可能的反弹期。为了调查是否出现(短暂的)反弹效应,在停止研究药物使用至少72小时后额外测量各项参数。在使用短效β2激动剂12周后,在最后一剂药物给药15小时(中位数)后测量,FEV1从预测值的85.6(±2.21)%降至78.8(±2.9)%。与安慰剂相比,这有显著差异。在168小时(中位数)后测量时,FEV1恢复到预测值的85.5(±2.4)%,与基线相当。在使用短效β2激动剂12周后,在最后一剂药物给药15小时后测量,PC20下降了-1.17(±0.44)倍剂量,与安慰剂相比有显著差异。然而,168小时后PC20略有恢复,增加了+0.55(±0.34)倍剂量,但该值仍低于安慰剂。相比之下,在使用长效β2激动剂和安慰剂期间未观察到显著变化。总之,使用短效β2激动剂会导致FEV出现短暂(反弹)效应,而对PC20的影响可能表明疾病出现了真正的恶化。使用长效β2激动剂和安慰剂未显示出变化。我们得出结论,短效而非长效β2激动剂的单一疗法可能对哮喘有有害影响。

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