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首页> 外文期刊>European Journal of Medicinal Chemistry: Chimie Therapeutique >Synthesis of spiro-2,6-dioxopiperazine and spiro-2,6-dioxopyrazine scaffolds using amino acids in a three-component reaction to generate potential Sigma-1 (sigma(1)) receptor selective ligands
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Synthesis of spiro-2,6-dioxopiperazine and spiro-2,6-dioxopyrazine scaffolds using amino acids in a three-component reaction to generate potential Sigma-1 (sigma(1)) receptor selective ligands

机译:用三组分反应中的氨基酸合成螺氧-2,6-二氧基哌嗪和螺旋-2,6-二氧基吡嗪支架以产生潜在的Sigma-1(Sigma(1))受体选择性配体

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摘要

A library-friendly approach to generate new scaffolds is decisive for the development of molecular probes, drug like molecules and preclinical entities. Here, we present the design and synthesis of novel heterocycles with spiro-2,6-dioxopiperazine and spiro-2,6-pyrazine scaffolds through a three component reaction using various amino acids, ketones, and isocyanides. Screening of select compounds over fifty CNS receptors including G-protein coupled receptors (GPCRs), ion channels, transporters, and enzymes through the NIMH psychoactive drug screening program indicated that a novel spiro-2,6-dioxopyrazine scaffold, UVM147, displays high binding affinity at sigma-1 (sigma(1)) receptor in the nanomolar range. In addition, molecular docking of UVM147 at the human sigma(1) receptor have shown that it resides in the same binding site that was occupied by the ligand 4-IBP used to obtain a crystal structure of the human sigma-1 (sigma(1)) receptor. (C) 2018 Elsevier Masson SAS. All rights reserved.
机译:生成新支架的图书馆友好的方法是对分子探针,药物和临床前实体的发展的决定性。在这里,我们通过使用各种氨基酸,酮和异氰酸酯,通过三种组分反应介绍与螺二氧吡啶哌嗪和螺螺杆-2,6-吡嗪支架的新杂环的设计和合成。通过NiMH精神活性药物筛查程序的筛选包括G-蛋白偶联受体(GPCR),离子通道,转运蛋白和酶,包括G-蛋白偶联受体(GPCR),离子通道,转运蛋白和酶的选择化合物表明了一种新的螺旋-2,6-二氧杂氮杂物支架,UVM147,显示出高结合在纳米罗拉范围内的Sigma-1(Sigma(1))受体的亲和力。此外,在人Sigma(1)受体处的UVM147的分子对接表明,它在与用于获得人类Sigma-1的晶体结构的配体4-IBP占据的相同结合位点中(Sigma(1 ))受体。 (c)2018年Elsevier Masson SAS。版权所有。

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