介导人离体子宫动脉收缩和舒张的前列腺素受体的特性研究

Characterization of the prostanoid receptors mediating constriction and relaxation of human isolated uterine artery.

作者信息

Baxter G S, Clayton J K, Coleman R A, Marshall K, Sangha R, Senior J

机构信息

Neurology Research Department, Smithkline Beecham Pharmaceuticals, New Frontiers Science Park, Harlow, Essex.

出版信息

Br J Pharmacol. 1995 Sep;116(1):1692-6. doi: 10.1111/j.1476-5381.1995.tb16393.x.

DOI:10.1111/j.1476-5381.1995.tb16393.x

PMID:8564239

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1908906/

Abstract

This study was undertaken to characterize pharmacologically the prostanoid receptor subtypes mediating constriction and relaxation of human isolated uterine artery. 2. U-46619 was a potent constrictor agonist on human uterine artery (EC50 [95% CL] = 3.5 [1.8-6.7] nM). Prostaglandin E2 (PGE2), PGF2 alpha, PGD2 and PGI2 only weakly constricted the uterine artery, being at least 100 times less potent than U-46619. The PGE2 and PGI2 constrictor effects may be modified by the potent dilator effects of these compounds. A number of agonists which show selectivity for FP-, DP- and EP-receptors including ICI 81008, BW 245C, sulprostone, rioprostil and butaprost, failed to cause any constriction at concentrations up to 30 microM. 3. Constrictor responses induced by all agonists tested were reduced or abolished by the TP-receptor blocking drugs, GR 32191 and EP 092. pA2 estimates for both antagonists versus U-46619 were 8.50, values which are consistent with their affinities at TP-receptors. 4. In preparations pre-constricted with phenylephrine (1 microM) both PGI2 and PGE2 were potent relaxant agonists. The selective IP-receptor agonists, cicaprost and iloprost, also dilated human uterine artery and were approximately 10 fold more potent than PGI2. The EP2-receptor agonists, butaprost and rioprostil and the selective DP-agonist, BW 245C, were at least 100 fold weaker than PGI2 and PGE2 suggesting that neither DP- nor EP2 receptors were involved. 5. We conclude that TP-receptors mediate constriction, whereas IP- and possibly EP4-receptors mediate relaxation of human uterine artery.

摘要

本研究旨在从药理学角度对介导人离体子宫动脉收缩和舒张的前列腺素受体亚型进行表征。2. U - 46619是一种对人子宫动脉有强效收缩作用的激动剂（EC50[95%可信区间]=3.5[1.8 - 6.7] nM）。前列腺素E2（PGE2）、前列腺素F2α、前列腺素D2和前列环素（PGI2）对子宫动脉的收缩作用较弱，效力至少比U - 46619低100倍。PGE2和PGI2的收缩作用可能会被这些化合物的强效舒张作用所改变。许多对FP、DP和EP受体具有选择性的激动剂，包括ICI 81008、BW 245C、舒前列素、利奥前列素和布他前列素，在浓度高达30 microM时均未引起任何收缩。3. 所有测试激动剂诱导的收缩反应均被TP受体阻断药物GR 32191和EP 092降低或消除。两种拮抗剂对U - 46619的pA2估计值均为8.50，该值与其在TP受体上的亲和力一致。4. 在预先用去氧肾上腺素（1 microM）预收缩的制剂中，PGI2和PGE2均为强效舒张激动剂。选择性IP受体激动剂西卡前列素和伊洛前列素也能舒张人子宫动脉，效力比PGI2高约10倍。EP2受体激动剂布他前列素和利奥前列素以及选择性DP激动剂BW 245C的效力至少比PGI2和PGE2弱100倍，这表明DP和EP2受体均未参与。5. 我们得出结论，TP受体介导收缩，而IP受体以及可能的EP4受体介导人子宫动脉的舒张。

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介导人离体子宫动脉收缩和舒张的前列腺素受体的特性研究

Characterization of the prostanoid receptors mediating constriction and relaxation of human isolated uterine artery.

作者信息

Baxter G S, Clayton J K, Coleman R A, Marshall K, Sangha R, Senior J

机构信息

Neurology Research Department, Smithkline Beecham Pharmaceuticals, New Frontiers Science Park, Harlow, Essex.

出版信息

Br J Pharmacol. 1995 Sep;116(1):1692-6. doi: 10.1111/j.1476-5381.1995.tb16393.x.

DOI:10.1111/j.1476-5381.1995.tb16393.x

PMID:8564239

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1908906/

Abstract

This study was undertaken to characterize pharmacologically the prostanoid receptor subtypes mediating constriction and relaxation of human isolated uterine artery. 2. U-46619 was a potent constrictor agonist on human uterine artery (EC50 [95% CL] = 3.5 [1.8-6.7] nM). Prostaglandin E2 (PGE2), PGF2 alpha, PGD2 and PGI2 only weakly constricted the uterine artery, being at least 100 times less potent than U-46619. The PGE2 and PGI2 constrictor effects may be modified by the potent dilator effects of these compounds. A number of agonists which show selectivity for FP-, DP- and EP-receptors including ICI 81008, BW 245C, sulprostone, rioprostil and butaprost, failed to cause any constriction at concentrations up to 30 microM. 3. Constrictor responses induced by all agonists tested were reduced or abolished by the TP-receptor blocking drugs, GR 32191 and EP 092. pA2 estimates for both antagonists versus U-46619 were 8.50, values which are consistent with their affinities at TP-receptors. 4. In preparations pre-constricted with phenylephrine (1 microM) both PGI2 and PGE2 were potent relaxant agonists. The selective IP-receptor agonists, cicaprost and iloprost, also dilated human uterine artery and were approximately 10 fold more potent than PGI2. The EP2-receptor agonists, butaprost and rioprostil and the selective DP-agonist, BW 245C, were at least 100 fold weaker than PGI2 and PGE2 suggesting that neither DP- nor EP2 receptors were involved. 5. We conclude that TP-receptors mediate constriction, whereas IP- and possibly EP4-receptors mediate relaxation of human uterine artery.

摘要

本研究旨在从药理学角度对介导人离体子宫动脉收缩和舒张的前列腺素受体亚型进行表征。2. U - 46619是一种对人子宫动脉有强效收缩作用的激动剂（EC50[95%可信区间]=3.5[1.8 - 6.7] nM）。前列腺素E2（PGE2）、前列腺素F2α、前列腺素D2和前列环素（PGI2）对子宫动脉的收缩作用较弱，效力至少比U - 46619低100倍。PGE2和PGI2的收缩作用可能会被这些化合物的强效舒张作用所改变。许多对FP、DP和EP受体具有选择性的激动剂，包括ICI 81008、BW 245C、舒前列素、利奥前列素和布他前列素，在浓度高达30 microM时均未引起任何收缩。3. 所有测试激动剂诱导的收缩反应均被TP受体阻断药物GR 32191和EP 092降低或消除。两种拮抗剂对U - 46619的pA2估计值均为8.50，该值与其在TP受体上的亲和力一致。4. 在预先用去氧肾上腺素（1 microM）预收缩的制剂中，PGI2和PGE2均为强效舒张激动剂。选择性IP受体激动剂西卡前列素和伊洛前列素也能舒张人子宫动脉，效力比PGI2高约10倍。EP2受体激动剂布他前列素和利奥前列素以及选择性DP激动剂BW 245C的效力至少比PGI2和PGE2弱100倍，这表明DP和EP2受体均未参与。5. 我们得出结论，TP受体介导收缩，而IP受体以及可能的EP4受体介导人子宫动脉的舒张。

介导人离体子宫动脉收缩和舒张的前列腺素受体的特性研究

Characterization of the prostanoid receptors mediating constriction and relaxation of human isolated uterine artery.

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介导人离体子宫动脉收缩和舒张的前列腺素受体的特性研究

Characterization of the prostanoid receptors mediating constriction and relaxation of human isolated uterine artery.

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出版信息