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甘丙肽(2-11)在转染细胞系中与GalR3结合:受体亚型药理学定义的局限性

Galanin (2-11) binds to GalR3 in transfected cell lines: limitations for pharmacological definition of receptor subtypes.

作者信息

Lu Xiaoying, Lundström Linda, Bartfai Tamas

机构信息

Department of Neuropharmacology, The Harold L. Dorris Neurological Research Center, The Scripps Research Institute, 10550 North Torrey Pines Road, La Jolla, CA 92037, USA.

出版信息

Neuropeptides. 2005 Jun;39(3):165-7. doi: 10.1016/j.npep.2004.12.013. Epub 2005 Feb 1.

Abstract

The neuropeptide galanin regulates a variety of physiological and pathophysiological processes through three G protein coupled receptors, GalR1, GalR2, and GalR3. The studies on galanin receptor subtype specific effects have been hampered by the lack of high affinity subtype selective antagonist and/or agonist to any of these three galanin receptor subtypes. Since its recent introduction in 2003, galanin (2-11) has been widely used as a GalR2 selective agonist in several in vitro and in vivo studies. In the present paper, we demonstrate that galanin (2-11) binds to rat GalR3 receptors in transfected cell lines with a similar affinity as it binds to GalR2. As none of the available antagonists are galanin receptor subtype selective, as shown here for M35 and M40, more work is needed to confirm whether a galanin (2-11) effect is GalR2 mediated and there is an urgent need for high affinity galanin receptor subtype selective ligands. For now one needs to interpret the data obtained at lower galanin (2-11) concentrations as effects mediated by non-GalR1 type galanin receptors, i.e., GalR2 and/or GalR3.

摘要

神经肽甘丙肽通过三种G蛋白偶联受体GalR1、GalR2和GalR3调节多种生理和病理生理过程。由于缺乏对这三种甘丙肽受体亚型中任何一种具有高亲和力的亚型选择性拮抗剂和/或激动剂,对甘丙肽受体亚型特异性作用的研究受到了阻碍。自2003年其最近被引入以来,甘丙肽(2-11)已在多项体外和体内研究中被广泛用作GalR2选择性激动剂。在本文中,我们证明甘丙肽(2-11)在转染细胞系中与大鼠GalR3受体结合,其亲和力与它与GalR2结合时相似。由于现有的拮抗剂都不是甘丙肽受体亚型选择性的,如这里所示的M35和M40,需要更多的工作来确认甘丙肽(2-11)的作用是否由GalR2介导,并且迫切需要高亲和力的甘丙肽受体亚型选择性配体。目前,人们需要将在较低甘丙肽(2-11)浓度下获得的数据解释为由非GalR1型甘丙肽受体介导的作用,即GalR2和/或GalR3。

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