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沙丁胺醇、色甘酸钠和异丙托溴铵对哮喘患者气道及循环介质对变应原支气管激发反应的影响。

Influence of albuterol, cromolyn sodium and ipratropium bromide on the airway and circulating mediator responses to allergen bronchial provocation in asthma.

作者信息

Howarth P H, Durham S R, Lee T H, Kay A B, Church M K, Holgate S T

出版信息

Am Rev Respir Dis. 1985 Nov;132(5):986-92. doi: 10.1164/arrd.1985.132.5.986.

Abstract

The effect of pharmacologic agents on mast cell mediator release was investigated in vivo. Eight atopic asthmatic subjects with airways relatively unreactive to nonspecific stimuli (geometric mean PC20 methacholine, 4.0 mg/ml) underwent single-concentration allergen challenge before (control) or after inhaling albuterol 200 micrograms, cromolyn sodium 20 mg, or 0.9% sodium chloride placebo. Six of the same subjects also underwent allergen challenge after pretreatment with ipratropium bromide, 1 mg. Airway responses to pharmacologic agents and bronchial challenge were measured by change in both specific airway conductance (SGaw) and FEV1. Mast cell mediator release was monitored by serial change in plasma histamine and, in addition, serum neutrophil chemotactic factor (NCF) on the placebo, albuterol, and cromolyn sodium challenge days. Control and placebo allergen challenges were associated with repeatable mean maximal falls in SGaw (48.5 versus 49.6%) and FEV1 (25.7 versus 25.5%). The mean increments in plasma histamine were not significantly different on the control (0.17 to 0.44 ng/ml) or placebo challenge days (0.18 to 0.64 ng/ml), with maximal levels occurring 5 min after challenge. A sustained increase in NCF was identified on the placebo challenge day (155.0% above baseline). Pretreatment with albuterol abolished any significant bronchoconstriction, with mean maximal falls in SGaw and FEV1 after challenge of 7.5 and 1.4%, respectively. These changes in airway caliber were not associated with any significant increment in mean plasma histamine (0.17 to 0.22 ng/ml) or serum NCF (4.1% increase). Cromolyn sodium pretreatment, while attenuating the airway response, was still associated with significant falls in SGaw (22.7%) and FEV1 (7.3%) and increases in plasma histamine (0.18 to 0.27 ng/ml).(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

在体内研究了药物制剂对肥大细胞介质释放的影响。八名对非特异性刺激气道反应相对不敏感的特应性哮喘患者(乙酰甲胆碱PC20几何平均值为4.0mg/ml)在吸入200微克沙丁胺醇、20mg色甘酸钠或0.9%氯化钠安慰剂之前(对照)或之后接受单浓度变应原激发试验。相同的六名受试者在使用1mg异丙托溴铵预处理后也接受了变应原激发试验。通过比气道传导率(SGaw)和第一秒用力呼气容积(FEV1)的变化来测量气道对药物制剂和支气管激发试验的反应。通过血浆组胺的系列变化以及在安慰剂、沙丁胺醇和色甘酸钠激发试验日血清中性粒细胞趋化因子(NCF)来监测肥大细胞介质释放。对照和安慰剂变应原激发试验与SGaw(48.5%对49.6%)和FEV1(25.7%对25.5%)可重复的平均最大下降相关。对照激发试验日(0.17至0.44ng/ml)或安慰剂激发试验日(0.18至0.64ng/ml)血浆组胺的平均增量无显著差异,最大水平出现在激发后5分钟。在安慰剂激发试验日发现NCF持续增加(比基线高155.0%)。沙丁胺醇预处理消除了任何显著的支气管收缩,激发后SGaw和FEV1的平均最大下降分别为7.5%和1.4%。气道管径的这些变化与平均血浆组胺(0.17至0.22ng/ml)或血清NCF的任何显著增加(增加4.1%)无关。色甘酸钠预处理虽然减弱了气道反应,但仍与SGaw显著下降(22.7%)和FEV1下降(7.3%)以及血浆组胺增加(0.18至0.27ng/ml)相关。(摘要截短至250字)

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