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首页> 外文期刊>Journal of Medicinal Chemistry >2-N-acylaminoalkylindoles: design and quantitative structure-activity relationship studies leading to MT2-selective melatonin antagonists.
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2-N-acylaminoalkylindoles: design and quantitative structure-activity relationship studies leading to MT2-selective melatonin antagonists.

机译:2-N-酰基氨基烷基吲哚:设计和定量构效关系研究导致MT2选择性褪黑激素拮抗剂。

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摘要

Several indole analogues of melatonin (MLT) were obtained by moving the MLT side chain from C(3) to C(2) of the indole ring. Binding and in vitro functional assays were performed on cloned human MT1 and MT2 receptors, stably transfected in NIH3T3 cells. Quantitative structure-activity relationship studies showed that 4-methoxy-2-(N-acylaminomethyl)indoles, with a benzyl group in position 1, were selective MT2 antagonists and, in particular, N-[(1-p-chlorobenzyl-4-methoxy-1H-indol-2-yl)methyl]propanamide (12) behaved as a pure antagonist at MT1 and MT2 receptors, with a 148-fold selectivity for MT2. We present a topographical model that suggests a lipophilic group, located out of the plane of the indole ring of MLT, as the key feature of the MT2 selective antagonists.
机译:通过将MLT侧链从吲哚环的C(3)移动到C(2),可获得褪黑激素(MLT)的几种吲哚类似物。对克隆的人MT1和MT2受体进行了结合和体外功能测定,这些受体在NIH3T3细胞中稳定转染。定量构效关系研究表明,在1位具有苄基的4-甲氧基-2-(N-酰基氨基甲基)吲哚是选择性的MT2拮抗剂,尤其是N-[(1-p-chloro苄基-4-甲氧基-1H-吲哚-2-基)甲基]丙酰胺(12)在MT1和MT2受体上表现为纯拮抗剂,对MT2的选择性为148倍。我们提出了一种地形模型,该模型表明了一个亲脂性基团,它位于MLT吲哚环的平面之外,是MT2选择性拮抗剂的关键特征。

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