首页> 外文期刊>European Journal of Medicinal Chemistry: Chimie Therapeutique >Interaction of novel condensed triazine derivatives with central and peripheral type benzodiazepine receptors: synthesis, in vitro pharmacology and modelling.
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Interaction of novel condensed triazine derivatives with central and peripheral type benzodiazepine receptors: synthesis, in vitro pharmacology and modelling.

机译:新型缩合三嗪衍生物与中枢和外围型苯并二氮杂receptor受体的相互作用:合成,体外药理和建模。

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摘要

Structurally related sets of triazino-quinoline, triazino-isoquinoline and pyrido-triazine derivatives were synthesised and their binding interactions with central (CBR)- and peripheral-type (PBR) benzodiazepine binding sites have been characterised. Of 33 compounds tested, a new compound, 2-(4-methylphenyl)-3H- [1,2,4] triazino [2, 3-a] quinolin-3-one (1 g) showed the lowest CBR binding inhibition constant (K(i) = 42 +/- 9 nM) and the highest CBR over PBR selectivity (>1300). All but the 4-methylphenyl (1 g) structural modifications decreased the affinity and selectivity of the parent compound, 2-phenyl-3H- [1,2,4]triazino[2,3-a]quinolin-3-one (1d) (K(i) = 69 +/- 9 nM, selectivity >890). Molecular interactions between selected ligands (standards and triazine derivatives) and alpha(1)gamma(2) subunit-interface residues in a GABA(A) receptor extracellular domain homology model have been calculated. Comparing data with calculations confirmed hydrogen bonding to gamma(2)Thr142 and hydrophobic interaction with alpha(1)His101 as being essential for high-affinity CBR binding.
机译:合成了结构上相关的三嗪基喹啉,三嗪基异喹啉和吡啶三嗪衍生物,并表征了它们与中心(CBR)型和外围型(PBR)苯并二氮杂结合位点的结合相互作用。在测试的33种化合物中,新化合物2-(4-甲基苯基)-3H- [1,2,4]三嗪基[2,3-a]喹啉-3-酮(1 g)显示出最低的CBR结合抑制常数(K(i)= 42 +/- 9 nM)和超过PBR选择性的最高CBR(> 1300)。除4-甲基苯基(1 g)以外的所有结构修饰均降低了母体化合物2-苯基-3H- [1,2,4]三嗪基[2,3-a]喹啉-3-酮(1d )(K(i)= 69 +/- 9 nM,选择性> 890)。已计算出所选配体(标准品和三嗪衍生物)与GABA(A)受体胞外域同源性模型中的alpha(1)gamma(2)亚基界面残基之间的分子相互作用。将数据与计算结果进行比较证实,氢与gamma(2)Thr142的键合以及与alpha(1)His101的疏水相互作用对于高亲和力CBR结合至关重要。

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