Intraocular pressure effects of selective prostanoid receptor agonists involve different receptor subtypes according to radioligand binding studies.

Journal of lipid mediators Pub Date : 1993-03-01
D F Woodward, R A Lawrence, C E Fairbairn, T Shan, L S Williams
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Abstract

The receptors involved in the ocular hypotensive activity of prostaglandins (PG) E2 and F2 alpha in dogs and monkeys was investigated by examining the effects of putative receptor selective agonists on intraocular pressure. A diverse variety of receptor selective agonists lowered intraocular pressure in these species. Thus, FP-receptor agonists (17-phenyl PGF2 alpha, fluprostenol), agonists with potent activity at the EP3 receptor (MB 28767, sulprostone) and a prostanoid with activity at the EP2 receptor (11-deoxy PGE1) were all potent ocular hypotensives when administered as a single dose to dogs and monkeys or b.i.d. for 5 days in monkeys. These findings were regarded as surprising and prompted us to re-examine some aspects of the current classification for prostanoid receptors. At present certain receptor subtypes, notably EP2, EP3 and FP receptors, are defined only according to the potency rank order for agonists. In these studies, we employed radioligand binding studies to determine the degree of competition between prostanoid agonists claimed to be selective on the basis of functional assays. Competition studies with a diverse variety of prostanoids at the binding site for PGE2 and sulprostone on the myometrial plasma membrane prepared from the rat uterus were consistent with the presence of an EP3 receptor. Thus, EP3-receptor agonists (MB 28767 and sulprostone) potently inhibited PGE2 and sulprostone binding, whereas FP agonists (17-phenyl PGF2 alpha, fluprostenol), a DP agonist (BW 245C), an EP1 antagonist (AH 6809), an EP2 agonist (AH 13205) and TP-receptor ligands (BM 13505, I-BOP) afforded little or no inhibition.(ABSTRACT TRUNCATED AT 250 WORDS)

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根据放射配体结合研究,选择性前列腺素受体激动剂对眼压的影响涉及不同的受体亚型。
通过观察几种受体选择性激动剂对眼压的影响,研究了犬和猴体内参与前列腺素(PG) E2和F2 α降眼压活性的受体。多种受体选择性激动剂可降低这些物种的眼压。因此,fp受体激动剂(17-苯基PGF2 α,氟前列腺醇),对EP3受体具有有效活性的激动剂(MB 28767,磺胺酮)和对EP2受体具有活性的前列腺素(11-deoxy PGE1)作为单剂量给药给狗和猴子或对猴子进行5天的b.d服用时,都是有效的降压药。这些发现被认为是令人惊讶的,并促使我们重新审视目前前列腺素受体分类的某些方面。目前,某些受体亚型,特别是EP2、EP3和FP受体,仅根据激动剂的效力等级顺序来定义。在这些研究中,我们采用放射配体结合研究来确定前列腺素激动剂之间的竞争程度,这些激动剂在功能分析的基础上声称具有选择性。在大鼠子宫肌层质膜上,多种前列腺素与PGE2和磺胺酮结合位点的竞争研究与EP3受体的存在一致。因此,ep3受体激动剂(MB 28767和磺胺酮)能有效抑制PGE2和磺胺酮的结合,而FP激动剂(17-苯基PGF2 α,氟前列腺醇),DP激动剂(BW 245C), EP1拮抗剂(AH 6809), EP2激动剂(AH 13205)和tp受体配体(BM 13505, I-BOP)几乎没有或没有抑制作用。(摘要删节250字)
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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