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来自犬类哮喘模型的气道平滑肌中的组胺药理学

Histamine pharmacology in airway smooth muscle from a canine model of asthma.

作者信息

Antonissen L A, Mitchell R W, Kroeger E A, Kepron W, Stephens N L, Bergen J

出版信息

J Pharmacol Exp Ther. 1980 Apr;213(1):150-5.

PMID:7359363
Abstract

Tracheal smooth muscle (TSM) from an ovalbumin sensitized canine model of allergic asthma showed hypersensitivity and hyper-reactivity to histamine (H) when compared to that from littermate controls in vitro. Mepyramine abolished H responses in TSM of both groups; it also abolished the allergic response to obalbumin of TSM from sensitized dogs. The H2 receptor agonist, 4-methyl histamine (4-MH) caused small dose-related decreases in H contractures but had no effect on carbachol- or K+-induced tension. Metiamide, an H2 antagonist, did not enhance the H contracture, suggesting the 4-MH may not be exerting a relaxant effect since H2 receptors were absent. The maximum H-induced isometric tension was potentiated when the sensitized and control muscle strips were pre-equilibrated with 4-MH. These observations are consistent with the presence in canine TSM of H1 but not relaxant H2 receptors, the release of endogenous H to the tissue during the antigen-antibody reaction, and the competition of H and 4-MH for the H1 receptors. Experiments with specific blockers also indicated that in this model the only transmitter found in the ovalbumin-induced allergic bronchospasm was histamine.

摘要

与同窝对照犬的气管平滑肌(TSM)相比,来自卵清蛋白致敏的过敏性哮喘犬模型的TSM在体外对组胺(H)表现出超敏反应和高反应性。美吡拉敏消除了两组TSM中的H反应;它还消除了致敏犬TSM对卵清蛋白的过敏反应。H2受体激动剂4-甲基组胺(4-MH)导致与剂量相关的H收缩小幅降低,但对卡巴胆碱或钾离子诱导的张力没有影响。H2拮抗剂甲硫咪特并未增强H收缩,这表明由于不存在H2受体,4-MH可能未发挥松弛作用。当用4-MH对致敏和对照肌条进行预平衡时,最大H诱导的等长张力增强。这些观察结果与犬TSM中存在H1受体而非具有松弛作用的H2受体、抗原-抗体反应期间内源性H释放到组织中以及H和4-MH对H1受体的竞争一致。使用特异性阻滞剂的实验还表明,在该模型中,卵清蛋白诱导的过敏性支气管痉挛中发现的唯一递质是组胺。

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