通过抑制环氧化酶-1和-2增加视网膜血管前列腺素受体功能。

Increases in retinovascular prostaglandin receptor functions by cyclooxygenase-1 and -2 inhibition.

作者信息

Hardy P, Bhattacharya M, Abran D, Peri K G, Asselin P, Varma D R, Chemtob S

机构信息

Department of Pediatrics, Research Center of Hôpital Sainte-Justine, Montreal, Quebec, Canada.

出版信息

Invest Ophthalmol Vis Sci. 1998 Sep;39(10):1888-98.

PMID:9727412

Abstract

PURPOSE

To determine the relative contribution of cyclooxygenase (COX)-1 and COX-2 in regulating prostaglandin (PG) E2 and PGF2alpha receptors (EP and FP, respectively) densities and their functions in retinal vasculature of neonatal pigs.

METHODS

Newborn pigs were treated intravenously every 8 hours for 48 hours with saline, 40 mg/kg nonselective COX inhibitor ibuprofen, 80 mg/kg COX-1 inhibitor valeryl salicylate, or 5 mg/kg DuP697 and 5 mg/kg NS398, COX-2 inhibitors. Retinal microvessel EP and FP receptor densities were measured by radioligand binding and receptor-coupled effects by determining second-messenger inositol 1,4,5-trisphosphate (IP3) and vasomotor responses. Retinal blood flow (RBF) response to incremental increases in blood pressure (BP) was measured by a microsphere technique.

RESULTS

Valeryl salicylate, DuP697, and NS398 reduced retinal PGE2 and PGF2alpha concentrations in the newborn by approximately half, whereas ibuprofen caused further reduction to levels observed in adults. Retinal vessel EP1, EP3, and FP receptor densities increased approximately threefold after treatments with COX-1 or COX-2 inhibitors, and five- to sixfold after ibuprofen treatment. EP and FP receptor upregulation was associated with corresponding increases in IP3 production and retinal vasoconstriction in response to PGF2alpha, fenprostalene (an FP agonist), PGE2, 17-phenyl trinor PGE2 (an EP1 agonist), and M&B28,767 (an EP3 agonist) and with enhanced RBF autoregulation of high BP (> or =125 mm Hg). Conversely, EP2 receptor density and coupled functions were minimally affected by COX inhibition.

CONCLUSIONS

Data suggest that increased COX-1- and COX-2-catalyzed prostaglandin synthesis contribute equivalently to the downregulation of retinovascular EP1, EP3, and FP receptors and their vasoconstrictor functions in newborn pigs; the EP2 receptor was not significantly influenced by ontogenic alterations in prostaglandin levels.

摘要

目的

确定环氧化酶（COX）-1和COX-2在调节新生猪视网膜血管中前列腺素（PG）E2和PGF2α受体（分别为EP和FP）密度及其功能方面的相对贡献。

方法

新生猪每隔8小时静脉注射一次，持续48小时，注射的药物分别为生理盐水、40mg/kg非选择性COX抑制剂布洛芬、80mg/kg COX-1抑制剂戊酰水杨酸酯，或5mg/kg DuP697和5mg/kg NS398（COX-2抑制剂）。通过放射性配体结合测定视网膜微血管EP和FP受体密度，并通过测定第二信使肌醇1,4,5-三磷酸（IP3）和血管舒缩反应来评估受体偶联效应。采用微球技术测量视网膜血流（RBF）对血压（BP）逐渐升高的反应。

结果

戊酰水杨酸酯、DuP697和NS398使新生猪视网膜中PGE2和PGF2α浓度降低约一半，而布洛芬则使其进一步降低至成年猪的水平。用COX-1或COX-2抑制剂处理后，视网膜血管EP1、EP3和FP受体密度增加约三倍，用布洛芬处理后增加五至六倍。EP和FP受体上调与IP3生成相应增加以及视网膜对PGF2α、芬前列林（一种FP激动剂）、PGE2、17-苯基三降PGE2（一种EP1激动剂）和M&B28,767（一种EP3激动剂）的血管收缩反应相关，并与高血压（≥125mmHg）时增强的RBF自身调节相关。相反，COX抑制对EP2受体密度及其偶联功能影响最小。