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OKY 1581对支气管收缩剂对花生四烯酸和PGH2反应的影响。

Effects of OKY 1581 on bronchoconstrictor responses to arachidonic acid and PGH2.

作者信息

Tilden S J, Underwood D C, Cowen K H, Wegmann M J, Graybar G B, Hyman A L, McNamara D B, Kadowitz P J

出版信息

J Appl Physiol (1985). 1987 May;62(5):2066-74. doi: 10.1152/jappl.1987.62.5.2066.

DOI:10.1152/jappl.1987.62.5.2066
PMID:2954941
Abstract

The influence of OKY 1581, a thromboxane synthase inhibitor, on airway responses to arachidonic acid and endoperoxide, [prostaglandin (PG) H2], were investigated in anesthetized, paralyzed, mechanically ventilated cats. Intravenous injections of arachidonic acid and PGH2 caused dose-related increases in transpulmonary pressure and lung resistance and decreases in dynamic and static compliance. OKY 1581 significantly decreased airway responses to arachidonic acid but not to PGH2. Sodium meclofenamate, a cyclooxygenase inhibitor, abolished airway responses to arachidonic acid but had no effect on airway responses to PGH2. OKY 1581 or meclofenamate has no effect on airway responses to PGF2 alpha, PGD2, or U 46619, a thromboxane mimic. In microsomal fractions from the lung, OKY 1581 inhibited thromboxane formation without decreasing prostacyclin synthesis or cyclooxygenase activity. These studies show that OKY 1581 is a selective thromboxane synthesis inhibitor in the cat lung and suggest that a substantial part of the bronchoconstrictor response to arachidonic acid is due to thromboxane A2 formation. Moreover, the present data suggest that airway responses to endogenously released and exogenous PGH2 are mediated differently and that a significant part of the response to exogenous PGH2 may be due to activation of an endoperoxide/thromboxane receptor, since responses to PGH2 are blocked by the thromboxane receptor antagonist SQ 29548.

摘要

在麻醉、麻痹、机械通气的猫身上,研究了血栓素合成酶抑制剂OKY 1581对气道对花生四烯酸和内过氧化物[前列腺素(PG)H2]反应的影响。静脉注射花生四烯酸和PGH2导致跨肺压和肺阻力呈剂量相关增加,动态和静态顺应性降低。OKY 1581显著降低了气道对花生四烯酸的反应,但对PGH2的反应没有影响。环氧化酶抑制剂甲氯芬那酸钠消除了气道对花生四烯酸的反应,但对气道对PGH2的反应没有影响。OKY 1581或甲氯芬那酸钠对气道对PGF2α、PGD2或血栓素类似物U 46619的反应没有影响。在肺微粒体部分,OKY 1581抑制血栓素形成,而不降低前列环素合成或环氧化酶活性。这些研究表明,OKY 1581是猫肺中的一种选择性血栓素合成抑制剂,并提示对花生四烯酸的支气管收缩反应的很大一部分是由于血栓素A2的形成。此外,目前的数据表明,气道对内源性释放和外源性PGH2的反应是通过不同机制介导的,并且对外源性PGH2反应的很大一部分可能是由于内过氧化物/血栓素受体的激活,因为对PGH2的反应被血栓素受体拮抗剂SQ 29548阻断。

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引用本文的文献

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Inhibition of pulmonary thromboxane A2 synthase activity and airway responses by CGS 13080.CGS 13080对肺血栓素A2合酶活性及气道反应的抑制作用
Mol Cell Biochem. 1989 Jan 23;85(1):29-41. doi: 10.1007/BF00223511.
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Actions of SQ 29,548 on contractile responses and arachidonic acid metabolism of intrapulmonary arteries, in vitro.
Agents Actions. 1992 Mar;35(3-4):280-8. doi: 10.1007/BF01997512.