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Receptors and signaling pathway underlying relaxations to isoprostanes in canine and porcine airway smooth muscle.

机译:犬和​​猪气道平滑肌松弛至异前列腺素的受体和信号通路。

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摘要

Using muscle bath techniques, we examined the inhibitory activities of several E- and F-ring isoprostanes in canine and porcine airway smooth muscle. 8-Isoprostaglandin E1 and 8-isoprostaglandin E2 (8-iso PGE2) reversed cholinergic tone in a concentration-dependent manner, whereas the F-ring isoprostanes were ineffective. Desensitization with 8-iso-PGE2 and PGE2 implicated isoprostane activity at the PGE2 receptor (EP). We found that the inhibitory E-ring isoprostane responses were significantly augmented by rolipram (a type IV phosphodiesterase inhibitor), while 1H-[1,2,4]-oxadiazolo[4,3-a]quinoxalin-1-one (a guanylate cyclase inhibitor) had no effect, suggesting a role for cAMP in isoprostane-mediated relaxations. 8-Iso-PGE2 did not reverse KCl tone, suggesting that voltage-dependent Ca2+ influx and myosin light chain kinase are not suppressed by isoprostanes. Patch-clamp studies showed marked suppression of K+ currents by 8-iso-PGE2. We conclude that E-ring isoprostanes exert PGE2 receptor-directed,cAMP-dependent relaxations in canine and porcine airway smooth muscle. This activity is not dependent on K+ channel activation or the direct inhibition of voltage-operated Ca2+ influx or myosin light chain kinase.
机译:使用肌肉沐浴技术,我们检查了几种E和F环异前列腺素在犬和猪气道平滑肌中的抑制活性。 8-异前列腺素E1和8-异前列腺素E2(8-异PGE2)以浓度依赖的方式逆转胆碱能的音调,而F环异前列腺素无效。用8-iso-PGE2和PGE2脱敏涉及在PGE2受体(EP)上的异前列腺素活性。我们发现,咯利普兰(IV型磷酸二酯酶抑制剂)显着增强了抑制性E环异前列腺素反应,而1H- [1,2,4]-恶二唑并[4,3-a]喹喔啉-1-酮(鸟苷酸环化酶抑制剂没有作用,提示cAMP在异前列腺素介导的松弛中起作用。 8-Iso-PGE2不能逆转KCl音调,表明电压依赖性Ca2 +内流和肌球蛋白轻链激酶不受异前列腺素抑制。膜片钳研究表明,8-iso-PGE2显着抑制了K +电流。我们得出的结论是,E环异前列腺素在犬和猪气道平滑肌中发挥PGE2受体导向的cAMP依赖性松弛作用。此活性不依赖于K +通道激活或电压操作的Ca 2+内流或肌球蛋白轻链激酶的直接抑制。

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