异应原诱导的豚鼠气管糖缀合物分泌:吲哚美辛、BW B70C和ZD-2138的调节作用

M. Yeadon, R.C. Price, Adrian N. Payne
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引用次数: 11

摘要

摘要:建立了一种测量麻醉、通气豚鼠气管分泌物的方法。上气管插管并灌注生理盐水。使用Lowry法分析灌注液中的蛋白质,通过从样品中的聚焦部分产生荧光团的程序分析糖缀合物(“粘液”)。静脉注射乙酰胆碱(ACh)刺激糖结合物分泌增加,在给药75 min后达到最大。总蛋白浓度未升高。静脉滴注15-HETE也能产生类似的糖缀合物分泌增加,但不增加蛋白质浓度,但最大作用时间比乙酰胆碱更早(30分钟)。在抗组胺预处理致敏动物中静脉输注过敏原(卵清蛋白)可诱导糖缀合物分泌,并在激射后30分钟达到峰值。吲哚美辛增强了过敏原诱导的糖缀合物分泌。据报道,5-脂氧合酶的特异性抑制剂ZD-2138可显著抑制过敏原诱导的肺支气管收缩,但不影响糖缀合物的分泌。相比之下,选择性5-,15-脂氧合酶抑制剂BW B70C可显著减轻过敏性气道关闭和糖缀合物分泌。这些研究证明了体内测定豚鼠气管中糖结合物分泌的可行性,以及乙酰胆碱和15-HETE是豚鼠体内有效的分泌物。此外,他们认为过敏性糖缀合物的分泌至少部分是通过脂质介质的释放而不是通过5-脂氧合酶介导的。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Allergen-induced Glycoconjugate Secretion in Guinea-pig Trachea in vivo: Modulation by Indomethacin, BW B70C and ZD-2138

Summary: A method has been established for measurement of tracheal secretions in anaesthetized, ventilated guinea-pigs. The upper trachea was cannulated and perfused with saline. The perfusate was analysed for protein using the Lowry assay and for glycoconjugates ('mucus') by a procedure generating a fluorophore from fucose moieties in the sample. Intravenously infused acetylcholine (ACh) stimulated an increase in glycoconjugate secretion which was maximal after 75 min of ACh administration. Total protein concentration was not increased. Intravenously infused 15-HETE produced a similar increase in glycoconjugate secretion also without increasing protein concentration, but the time of maximal effect was earlier (30 min) than with ACh. Intravenous infusion of allergen (ovalbumin) in antihistamine pretreated, sensitized animals induced a dose-related glycoconjugate secretion which was maximal at 30 min after challenge. Indomethacin potentiated allergen-induced glycoconjugate secretion. The reportedly specific inhibitor of 5-lipoxygenase, ZD-2138, substantially inhibited allergen-induced pulmonary bronchoconstriction but did not influence glycoconjugate secretion. In contrast, the selective 5-, 15-lipoxygenase inhibitor BW B70C significantly attenuated both allergic airway closure and glycoconjugate secretion. These studies demonstrate the practicability of measuring glycoconjugate secretion in guinea-pig trachea in vivo, and that ACh and 15-HETE are potent secretagogues in this species. Further, they suggest that allergic glycoconjugate secretion is mediated, at least in part, via the release of lipid mediators from pathways other than via 5-lipoxygenase.

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