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阿片类和黑皮质素受体:它们有重叠的药效基团吗?

Opioid and melanocortin receptors: do they have overlapping pharmacophores?

作者信息

Lee Yeon Sun, Agnes Richard S, Cain James P, Kulkarni Vinod, Cai Minying, Salibay Christine, Ciano Kathy, Petrov Ravil, Mayorov Alexander, Vagner Josef, Trivedi Dev, Davis Peg, Ma Shou-wu, Lai Josephine, Porreca Frank, Vardanyan Ruben, Hruby Victor J

机构信息

Department of Chemistry, University of Arizona, Tucson, AZ 85721, USA.

出版信息

Biopolymers. 2008;90(3):433-8. doi: 10.1002/bip.20814.

Abstract

We have identified compound 1 as a novel ligand for opioid and melanocortin (MC) receptors, which is derived from the overlapping of a well known structure for the delta opioid receptor, 2,6-dimethyltyrosine (Dmt)-1,2,3,4-tetrahydroisoquinoline-3-carboxylic acid (Tic), and a small molecule for the MC receptor, Tic-DPhe(p-Cl)-piperidin-4-yl-N-phenyl-propionamide. Ligand 1 showed that there is an overlapping pharmacophore between opioid and MC receptors through the Tic residue. The ligand displayed high biological activities at the delta opioid receptor (Ki = 0.38 nM in binding assay, EC(50) = 0.48 nM in GTP-gamma-S binding assay, IC(50) = 74 nM in MVD) as an agonist instead of an antagonist and showed selective binding affinity (IC(50) = 2.3 muM) at the MC-3 receptor rather than at the MC-5 receptor. A study of the structure-activity relationships demonstrated that the residues in positions 2, 3, and the C-terminus act as a pharmacophore for the MC receptors, and the residues in positions 1 and 2 act as a pharmacophore for the opioid receptors. Thus, this structural construct can be used to prepare chimeric structures with adjacent or overlapping pharmacophores for opioid and MC receptors.

摘要

我们已确定化合物1是一种新型的阿片样物质和黑皮质素(MC)受体配体,它源自δ阿片样物质受体的一种已知结构2,6 - 二甲基酪氨酸(Dmt)-1,2,3,4 - 四氢异喹啉 - 3 - 羧酸(Tic)与一种MC受体小分子Tic - D - Phe(p - Cl)- 哌啶 - 4 - 基 - N - 苯基丙酰胺的重叠。配体1表明,通过Tic残基,阿片样物质受体和MC受体之间存在重叠的药效基团。该配体作为激动剂而非拮抗剂,在δ阿片样物质受体上表现出高生物活性(结合试验中Ki = 0.38 nM,GTP - γ - S结合试验中EC(50) = 0.48 nM,MVD试验中IC(50) = 74 nM),并且在MC - 3受体而非MC - 5受体上表现出选择性结合亲和力(IC(50) = 2.3 μM)。构效关系研究表明,第2、3位残基和C末端作为MC受体的药效基团,第1和2位残基作为阿片样物质受体的药效基团。因此,这种结构构建体可用于制备具有相邻或重叠药效基团的阿片样物质受体和MC受体的嵌合结构。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/850d/2693099/75dc7cd6b3d1/nihms-112485-f0001.jpg

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