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首页> 外文期刊>American Journal of Physiology >Molecular and biochemical characterization of prostacyclin receptors in rat kidney.
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Molecular and biochemical characterization of prostacyclin receptors in rat kidney.

机译:大鼠肾脏中前列环素受体的分子和生化特征。

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摘要

The prostacyclin (IP) message was detected by RT-PCR in the renal cortex, outer (OM) and inner medulla (IM), and in freshly isolated (IMCD-f) and cultured inner medullary collecting duct (IMCD-c), and also the E-prostanoid (EP)1,3,4 receptor subtypes, but not EP2. Digoxigenin in situ hybridization localized IP mRNA in the tubules of the OM and IM, and the vasculature, and also in the glomeruli, arteries, and tubules of the cortex. IP splice variants or subtypes could not be detected by RT-PCR followed by TA cloning, though several nonfunctional point mutations or single base pair deletions were observed. Iloprost (ILP), cicaprost (CCP), PGE2, and arginine vasopressin (AVP) stimulated cAMP in both IMCD preparations. In addition, AVP-stimulated cAMP in IMCD-f was inhibited by all three prostanoids, but not in IMCD-c. Calcium experiments were performed on IMCD-c or microdissected IMCD (IMCD-m). CCP, ILP, and PGE2 did not alter intracellular calcium concentration ([Ca2+]i) in IMCD-c. However, on IMCD-m, both PGE2 and ILP increased [Ca2+]i levels equipotently and CCP had no effect. Pretreatment with the EP1 antagonist AH-6809 indicates that the response to ILP and PGE2 is mediated via EP1. These results suggest that IP receptors in the rat IMCD mediate the cAMP but not calcium signaling linked to PGI2; to date no subtypes or splice variants have been identified.
机译:通过RT-PCR在肾皮质,外部(OM)和内部髓质(IM),新鲜分离的(IMCD-f)和培养的内部髓质收集管(IMCD-c)中检测前列环素(IP)信息,以及也是E-前列腺素(EP)1、3、4受体亚型,但不是EP2。洋地黄毒苷原位杂交将IP mRNA定位于OM和IM的小管,脉管系统以及皮层的肾小球,动脉和小管中。尽管观察到一些非功能性点突变或单碱基对缺失,但RT-PCR和TA克隆法无法检测到IP剪接变体或亚型。两种IMCD制剂中,伊洛前列素(ILP),西卡前列素(CCP),PGE2和精氨酸加压素(AVP)均可刺激cAMP。此外,IMCD-f中AVP刺激的cAMP被所有三种类前列腺素抑制,而IMCD-c中没有。钙实验是在IMCD-c或显微解剖的IMCD(IMCD-m)上进行的。 CCP,ILP和PGE2不会改变IMCD-c中的细胞内钙浓度([Ca2 +] i)。但是,在IMCD-m上,PGE2和ILP均等地增加[Ca2 +] i水平,而CCP没有作用。用EP1拮抗剂AH-6809进行预处理表明,对ILP和PGE2的反应是通过EP1介导的。这些结果表明,大鼠IMCD中的IP受体介导cAMP,但不介导与PGI2相关的钙信号传导。迄今为止,尚未鉴定出亚型或剪接变体。

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