首页> 美国卫生研究院文献>British Journal of Pharmacology and Chemotherapy >Bronchodilator-mediated relaxation of normal and ovalbumin-sensitized guinea-pig airways: lack of correlation with lung adenylate cyclase activation.
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Bronchodilator-mediated relaxation of normal and ovalbumin-sensitized guinea-pig airways: lack of correlation with lung adenylate cyclase activation.

机译:支气管扩张剂介导的正常和卵白蛋白致敏的豚鼠气道舒张:与肺腺苷酸环化酶激活缺乏相关性。

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摘要

Isoprenaline, vasoactive intestinal peptide (VIP), prostaglandin E2 (PGE2) and forskolin caused a dose-dependent relaxation of normal and ovalbumin-sensitized guinea-pig tracheal spirals and lung parenchymal strips in vitro. There was no difference in magnitude of relaxation or sensitivity to these relaxants between normal and sensitized tissues. The rank order of potency (concentration of each drug at which 50% of the maximum is obtained) for these relaxants on both trachea and parenchyma was VIP greater than isoprenaline greater than PGE2 greater than forskolin, although the parenchyma was more sensitive than the trachea. The rank order of efficacy of the drugs used in relaxing both the trachea and lung parenchyma was isoprenaline (10 microM) greater than forskolin (30 microM) greater than VIP (0.1 microM) greater than PGE2 (10 microM). PGE2 at concentrations greater than 1 microM sometimes contracted the lung strip. Pretreatment with indomethacin (8.5 microM), a cyclo-oxygenase inhibitor, reduced the resting tone of tracheal spirals, but did not significantly affect the tone of lung strips. Indomethacin-pretreatment did not affect drug-induced relaxations of either normal or sensitized tracheal spirals. However, both normal and sensitized indomethacin-pretreated lung strips relaxed significantly less (P less than 0.05) to isoprenaline, PGE2 and forskolin. Indomethacin-pretreatment did not affect sensitivity of normal and sensitized trachea or parenchyma to the relaxant drugs. All the relaxant drugs used stimulated adenylate cyclase activity in normal or sensitized lung parenchyma membrane preparations. The rank order of efficacy (maximal activation) was forskolin greater than isoprenaline = VIP greater than PGE2. There was no difference in response between normal and sensitized lungs. Adenylate cyclase activity of normal lung was stimulated as follows: forskolin (100 microM), 500.0 +/- 50.0%; isoprenaline (100 microM), 186.0 +/- 29.0%; VIP (10 microM), 213.0 +/- 19.0% and PGE2 (100 microM), 155.0 +/- 23.0% of basal activity. Similar values were obtained for sensitized lung parenchyma. Indomethacin-pretreatment did not significantly affect normal or sensitized lung adenylate cyclase stimulation by isoprenaline, VIP, forskolin or PGE2. It was concluded that: Immunological sensitization to ovalbumin does not induce hypoactivity of relaxant drug receptors and/or the adenylate cyclase system of the airway tissues of the guinea-pig.(ABSTRACT TRUNCATED AT 400 WORDS)
机译:异丙肾上腺素,血管活性肠肽(VIP),前列腺素E2(PGE2)和福司可林在体外引起正常和卵白蛋白致敏的豚鼠气管螺旋和肺实质条带的剂量依赖性松弛。正常组织和致敏组织之间的松弛程度或对这些松弛剂的敏感性没有差异。这些松弛剂在气管和薄壁组织上的效价等级顺序(每种药物的浓度最高可达到50%)是VIP大于异丙肾上腺素大于PGE2大于福斯高林,尽管薄壁组织比气管更敏感。用于舒张气管和肺实质的药物的疗效等级排序是:异丙肾上腺素(10 microM)大于毛喉素(30 microM)大于VIP(0.1 microM)大于PGE2(10 microM)。浓度大于1 microM的PGE2有时会收缩肺带。用消炎痛(8.5 microM)(一种环加氧酶抑制剂)进行预处理可以降低气管螺旋的静息音,但不会显着影响肺带的音调。消炎痛预处理不影响药物引起的正常或致敏气管螺旋的松弛。但是,正常和致敏消炎痛预处理的肺条对异丙肾上腺素,PGE2和毛喉素的舒张作用均显着降低(P小于0.05)。消炎痛预处理不会影响正常和致敏的气管或实质对松弛药物的敏感性。在正常或致敏的肺实质膜制剂中,所有使用的松弛剂均能刺激腺苷酸环化酶活性。功效的等级顺序(最大激活)是福斯高林大于异丙肾上腺素= VIP大于PGE2。正常肺和致敏肺之间的反应没有差异。如下刺激正常肺的腺苷酸环化酶活性:福司可林(100 microM),500.0 +/- 50.0%;异丙肾上腺素(100 microM),186.0 +/- 29.0%; VIP(10 microM),213.0 +/- 19.0%和PGE2(100 microM),155.0 +/- 23.0%的基础活动。致敏的肺实质获得了相似的值。消炎痛预处理对异丙肾上腺素,VIP,福斯高林或PGE2刺激的正常或致敏的肺腺苷酸环化酶没有明显影响。结论是:对卵白蛋白的免疫敏化不会引起豚鼠气道组织的松弛药物受体和/或腺苷酸环化酶系统的功能减退(摘要截短为400字)。

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