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利用[3H]前列腺素E1结合法对犬小肠中前列腺素E受体的特性进行表征。

Characterization of prostaglandin E receptors in canine small intestine using [3H] prostaglandin E1 binding.

作者信息

Keith R H, Tsai B S, Collins P W, Perkins W E, Shone R L, Gasiecki A F, Bianchi R G, Bauer R F

机构信息

Immunoinflammatory Diseases Research, Searle, Skokie, IL 60077.

出版信息

Prostaglandins. 1992 Dec;44(6):579-95. doi: 10.1016/0090-6980(92)90026-p.

Abstract

Prostaglandin E (PGE) receptors in canine small intestinal mucosal and muscle membrane preparations were labeled with [3H] PGE1. Saturable, high affinity binding of [3H] PGE1 was observed in both preparations. The density of binding sites (fmol/mg protein) was 39 for mucosal membranes and 60 for muscle membranes, with corresponding dissociation constants of 10.6 nM and 5.8 nM, respectively. [3H] PGE1 binding sites in both preparations showed stereospecificity and high affinity for natural PGE1 and PGE2, but not for I or F-type PGs. Synthetic PGEs such as misoprostol and enisoprost had lower affinity than PGE1 or PGE2. Several analogs of enisoprost bound weakly to the binding sites. A highly significant correlation (C.C. = 0.9) was demonstrated between mucosal and muscle binding potency for a series of enisoprost analogs. There was also a significant positive correlation between the receptor binding potency and rat diarrheagenic activity for these analogs. These results indicate that PGE receptors in canine intestinal mucosa and muscle can be directly studied with [3H] PGE1 binding. The mucosal and muscle PGE receptors may have similar ligand binding specificity. We speculate that these receptors are likely to be associated with the diarrheagenic activity of PGEs.

摘要

用[³H]前列腺素E1(PGE1)标记犬小肠黏膜和肌膜制剂中的前列腺素E(PGE)受体。在两种制剂中均观察到[³H]PGE1的可饱和、高亲和力结合。黏膜膜结合位点的密度(fmol/mg蛋白质)为39,肌膜为60,相应的解离常数分别为10.6 nM和5.8 nM。两种制剂中的[³H]PGE1结合位点对天然PGE1和PGE2表现出立体特异性和高亲和力,但对I型或F型前列腺素(PGs)则不然。米索前列醇和依索前列醇等合成PGEs的亲和力低于PGE1或PGE2。依索前列醇的几种类似物与结合位点的结合较弱。一系列依索前列醇类似物的黏膜和肌肉结合能力之间存在高度显著的相关性(相关系数 = 0.9)。这些类似物的受体结合能力与大鼠致泻活性之间也存在显著的正相关。这些结果表明,可用[³H]PGE1结合直接研究犬肠道黏膜和肌肉中的PGE受体。黏膜和肌肉的PGE受体可能具有相似的配体结合特异性。我们推测这些受体可能与PGEs的致泻活性有关。

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