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白三烯调节剂在阿司匹林诱发哮喘中的保护作用。

The protective effects of leukotriene modifiers in aspirin-induced asthma.

作者信息

Israel E

机构信息

Pulmonary and Critical Care Division, Brigham and Women's Hospital, Boston, MA 02115, USA.

出版信息

Postgrad Med. 2000 Sep 15;108(4 Suppl):40-4. doi: 10.3810/pgm.09.15.2000.suppl7.291.

Abstract

Aspirin and other nonsteroidal anti-inflammatory drugs (NSAIDs) inhibit cyclooxygenase activity and, in aspirinintolerant patients, can precipitate life-threatening asthma attacks. In aspirin-sensitive asthmatic patients, exposure to aspirin results in a dramatic increase in cysteinyl leukotriene production, the precise mechanism of which remains unclear. However, clinical studies of the 2 types of leukotriene modifiers--the leukotriene synthesis inhibitors and the leukotriene receptor antagonists (LTRAs)--have established the critical pathogenic role played by leukotrienes in aspirin-induced asthma (AIA). Zileuton, the only leukotriene synthesis inhibitor now available, increased pulmonary function and alleviated the cardinal signs of AIA. Montelukast, a potent LTRA, blocked the airway obstruction induced by lysine-aspirin inhalation in aspirin-sensitive asthmatic patients. Pulmonary function improved significantly, and both ss-agonist use and frequency of nocturnal awakening decreased. Pranlukast, a LTRA available only in Japan, produced results similar to those reported for montelukast. Despite these agents' protective effects, aspirin-sensitive asthmatic patients should be cautioned to avoid the use of any drug that inhibits cyclooxygenase activity.

摘要

阿司匹林和其他非甾体抗炎药(NSAIDs)会抑制环氧化酶活性,对于阿司匹林不耐受的患者,可能引发危及生命的哮喘发作。在对阿司匹林敏感的哮喘患者中,接触阿司匹林会导致半胱氨酰白三烯生成显著增加,其确切机制尚不清楚。然而,对两种白三烯调节剂——白三烯合成抑制剂和白三烯受体拮抗剂(LTRAs)——的临床研究已证实白三烯在阿司匹林诱发的哮喘(AIA)中起关键致病作用。目前唯一可用的白三烯合成抑制剂齐留通可改善肺功能并缓解AIA的主要症状。强效LTRA孟鲁司特可阻断赖氨酸 - 阿司匹林吸入对阿司匹林敏感哮喘患者诱发的气道阻塞。肺功能显著改善,β受体激动剂的使用及夜间觉醒频率均降低。仅在日本可用的LTRA普仑司特产生了与孟鲁司特报道结果相似的效果。尽管这些药物具有保护作用,但仍应告诫对阿司匹林敏感的哮喘患者避免使用任何抑制环氧化酶活性的药物。

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