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强效血小板活化因子拮抗剂SR27417A对变应原诱导的哮喘反应的影响。

Effects of a potent platelet-activating factor antagonist, SR27417A, on allergen-induced asthmatic responses.

作者信息

Evans D J, Barnes P J, Cluzel M, O'Connor B J

机构信息

Clinical Studies Unit, Royal Brompton Hospital, London, United Kingdom.

出版信息

Am J Respir Crit Care Med. 1997 Jul;156(1):11-6. doi: 10.1164/ajrccm.156.1.9611112.

DOI:10.1164/ajrccm.156.1.9611112
PMID:9230719
Abstract

Platelet-activating factor (PAF) is a lipid-derived mediator that has been implicated in the pathophysiology of airway inflammation in asthma. Its actions include chemotaxis and activation of inflammatory cells, particularly eosinophils. Inhaled PAF causes bronchoconstriction and increased airway responsiveness in human subjects. However, PAF antagonists have so far failed to show benefits in allergen challenge or in the treatment of chronic asthma. SR27417A is a novel PAF antagonist with increased potency compared with previously tested compounds. Twelve asthmatic subjects received treatment with either SR27417A or placebo for 1 wk in a double-blind crossover study. After treatment each subject underwent allergen challenge. Effects were assessed in terms of early and late asthmatic responses and allergen-induced effects on airway responsiveness. Baseline lung function and airway responsiveness were also examined. Treatment with SR27417A significantly attenuated the late asthmatic response (AUC LAR4-10h: 107 +/- 24 after placebo, 79 +/- 17 after SR27417A, p < 0.05; mean maximal percent fall in FEV1 LAR: 29 +/- 6% after placebo, 23.5 +/- 5.4% after SR27417A, p < 0.05). There were no effects on early asthmatic responses, allergen-induced airway responsiveness, or baseline lung measurements. SR27417A is the most potent PAF antagonist to date, and it has a modest inhibitory effect on the late asthmatic response. This suggests that PAF has a small role in allergic inflammation.

摘要

血小板活化因子(PAF)是一种脂质衍生介质,与哮喘气道炎症的病理生理学有关。其作用包括趋化作用和炎症细胞(尤其是嗜酸性粒细胞)的激活。吸入PAF会导致人体受试者支气管收缩和气道反应性增加。然而,迄今为止,PAF拮抗剂在变应原激发试验或慢性哮喘治疗中均未显示出益处。与先前测试的化合物相比,SR27417A是一种新型PAF拮抗剂,其效力有所增强。在一项双盲交叉研究中,12名哮喘受试者接受了SR27417A或安慰剂治疗1周。治疗后,每位受试者均接受变应原激发试验。根据早期和晚期哮喘反应以及变应原诱导的气道反应性影响来评估效果。还检查了基线肺功能和气道反应性。SR27417A治疗显著减轻了晚期哮喘反应(安慰剂组4至10小时的晚期哮喘反应曲线下面积:107±24,SR27417A组为79±17,p<0.05;晚期哮喘反应中第一秒用力呼气容积的平均最大下降百分比:安慰剂组为29±6%,SR27417A组为23.5±5.4%,p<0.05)。对早期哮喘反应、变应原诱导的气道反应性或基线肺测量值均无影响。SR27417A是迄今为止效力最强的PAF拮抗剂,对晚期哮喘反应有适度的抑制作用。这表明PAF在过敏性炎症中作用较小。

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