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受体鸟苷酸环化酶报告细胞系的药理学特征。

Pharmacological characterization of receptor guanylyl cyclase reporter cell lines.

机构信息

Lead Discovery Wuppertal, Bayer HealthCare AG, Pharma Research Center, Aprather Weg 18a, Wuppertal D-42096, Germany.

出版信息

Eur J Pharmacol. 2013 Jan 5;698(1-3):131-6. doi: 10.1016/j.ejphar.2012.11.009. Epub 2012 Nov 21.

Abstract

Receptor guanylyl cyclases are implicated in a growing number of pathophysiologies and, therefore, represent an important target class for drug development. We report here the generation and pharmacological characterization of three particulate guanylyl cyclase (pGC) reporter cell lines. Plasmid constructs encoding the natriuretic peptide receptors GC-A and GC-B, and the heat-stable enterotoxin receptor GC-C, were stably transfected in a parental reporter cell line expressing a cyclic nucleotide-gated (CNG) cation channel, acting as the biosensor for intracellular cGMP. In our reporter cell lines pGC activity can be monitored in living cells in real-time . By using different natural as well as synthetic receptor ligands of the natriuretic and guanylin peptide families, we show that our reporter assay monitors pGC activity with very high sensitivity. In contrast to previous findings, we could detect significant stimulation of GC-A and GC-B by each of the natriuretic peptides ANP, BNP and CNP. In addition, the clearance receptor ligand Cys-ANF(4-18) and the ANP receptor antagonist Arg-ANF(6-18) were characterized as partial GC-A agonists. The results imply that our novel pGC reporter cell lines are well suited for the characterization of receptor pharmacology and may be used for natural ligand characterization of guanylyl cyclase orphan receptors.

摘要

受体鸟苷酸环化酶参与了越来越多的病理生理学过程,因此代表了药物开发的一个重要目标类别。我们在这里报告三种颗粒状鸟苷酸环化酶(pGC)报告细胞系的产生和药理学特征。编码利钠肽受体 GC-A 和 GC-B 以及热稳定肠毒素受体 GC-C 的质粒构建体稳定转染到表达环核苷酸门控(CNG)阳离子通道的亲本报告细胞系中,作为细胞内 cGMP 的生物传感器。在我们的报告细胞系中,可以实时监测活细胞中的 pGC 活性。通过使用利钠肽和鸟苷素肽家族的不同天然和合成受体配体,我们表明我们的报告测定法以非常高的灵敏度监测 pGC 活性。与先前的发现相反,我们能够检测到每种利钠肽 ANP、BNP 和 CNP 对 GC-A 和 GC-B 的显著刺激。此外,清除受体配体 Cys-ANF(4-18)和 ANP 受体拮抗剂 Arg-ANF(6-18)被表征为部分 GC-A 激动剂。结果表明,我们的新型 pGC 报告细胞系非常适合受体药理学的表征,并且可用于鸟苷酸环化酶孤儿受体的天然配体表征。

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