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兔前列腺素EP3受体mRNA的原位杂交及定位

In situ hybridization and localization of mRNA for the rabbit prostaglandin EP3 receptor.

作者信息

Breyer M D, Jacobson H R, Davis L S, Breyer R M

机构信息

Department of Veterans Affairs Medical Center, Vanderbilt University, Nashville, Tennessee.

出版信息

Kidney Int. 1993 Dec;44(6):1372-8. doi: 10.1038/ki.1993.391.

Abstract

The physiological effects of PGE2 appear to be mediated by at least three different "E-prostanoid" receptors designated EP1,EP2, and EP3. These receptors are differentially activated by structural PGE analogs (such as misoprostol) and each couples to a different signal transduction mechanism. Studies demonstrating that inhibition of water absorption in the collecting duct is mediated by a Gi coupled mechanism, suggests that an EP3 receptor is involved the renal effects of PGE2. We used in situ hybridization to determine the tissue distribution of the rabbit EP3 receptor. [alpha-35S] UTP labeled antisense RNA, comprising transmembrane domains IV through VII, was hybridized to tissue sections. Specific labeling of kidney, stomach and adrenal was observed. In the kidney, medullary thick ascending limb and cortical and medullary collecting ducts were intensely labeled, while no labeling of glomeruli, proximal tubules, or cortical thick ascending limbs was observed. The adrenal gland labeled exclusively in the medulla. In the stomach the gastric epithelial crypts were the predominant site of hybridization, without evidence of labeling of the smooth muscle. These results suggest an important role for the EP3 receptor in mediating PGE2 effects in these tissues.

摘要

前列腺素E2(PGE2)的生理效应似乎至少由三种不同的“E-前列腺素”受体介导,分别命名为EP1、EP2和EP3。这些受体被结构型PGE类似物(如米索前列醇)以不同方式激活,且各自与不同的信号转导机制偶联。有研究表明,集合管中水重吸收的抑制是由Gi偶联机制介导的,这提示EP3受体参与了PGE2的肾脏效应。我们采用原位杂交技术来确定兔EP3受体的组织分布。将包含跨膜结构域IV至VII的[α-35S]UTP标记反义RNA与组织切片进行杂交。观察到肾脏、胃和肾上腺有特异性标记。在肾脏中,髓质厚升支以及皮质和髓质集合管有强烈标记,而肾小球、近端小管或皮质厚升支未观察到标记。肾上腺仅在髓质有标记。在胃中,胃上皮隐窝是杂交的主要部位,平滑肌未见标记。这些结果表明EP3受体在介导PGE2在这些组织中的效应方面具有重要作用。

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