首页> 外文期刊>Journal of Medicinal Chemistry >From 2‑Triethylammonium Ethyl Ether of 4‑Stilbenol (MG624) to Selective Small-Molecule Antagonists of Human α9α10 Nicotinic Receptor by Modifications at the Ammonium Ethyl Residue
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From 2‑Triethylammonium Ethyl Ether of 4‑Stilbenol (MG624) to Selective Small-Molecule Antagonists of Human α9α10 Nicotinic Receptor by Modifications at the Ammonium Ethyl Residue

机译:从4-二苯酚(MG624)的2-三乙基铵乙醚到人α9α10烟碱受体的选择性小分子拮抗剂,通过对乙基铵残基的修饰

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摘要

Nicotinic acetylcholine receptors containing α9 subunits (α9*-nAChRs) are potential druggable targets arousing great interest for pain treatment alternative to opioids. Nonpeptidic small molecules selectively acting as α9*-nAChRs antagonists still remain an unattained goal. Here, through modifications of the cationic head and the ethylene linker, we have converted the 2-triethylammonium ethyl ether of 4-stilbenol (MG624), a well-known α7- and α9*-nAChRs antagonist, into some selective antagonists of human α9*-nAChR. Among these, the compound with cyclohexyldimethylammonium head (7) stands out for having no α7-nAChR agonist or antagonist effect along with very low affinity at both α7- and α3β4-nAChRs. At supra-micromolar concentrations, 7 and the other selective α9* antagonists behaved as partial agonists at α9*-nAChRs with a very brief response, followed by rebound current once the application is stopped and the channel is disengaged. The small or null postapplication activity of ACh seems to be related to the slow recovery of the rebound current.
机译:含有α9亚基(α9*-nAChRs)的烟碱乙酰胆碱受体是潜在的成药靶点,引起了人们对替代阿片类药物的疼痛治疗的极大兴趣。选择性地充当α9*-nAChRs拮抗剂的非肽小分子仍然是一个未实现的目标。在这里,通过对阳离子头和乙烯接头的修饰,我们将著名的α7-和α9*-nAChR拮抗剂4-二苯酚(MG624)的2-三乙基铵乙醚转化为人α9*-nAChR的一些选择性拮抗剂。其中,环己基二甲基铵头化合物 (7) 的突出特点是没有 α7-nAChR 激动剂或拮抗剂作用,并且在 α7- 和 α3β4-nAChR 上的亲和力都非常低。在超微摩尔浓度下,7 和其他选择性 α9* 拮抗剂在 α9*-nAChR 处表现为部分激动剂,反应非常短暂,一旦应用停止且通道脱离,就会产生反弹电流。ACh的少量或零应用后活性似乎与回弹电流恢复缓慢有关。

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