4-quinolone derivatives: High-affinity ligands at the benzodiazepine site of brain GABA(A) receptors. synthesis, pharmacology, and pharmacophore modeling

Lager E; Andersson P; Nilsson J; Pettersson I; Nielsen EO; Nielsen M; Sterner O; Liljefors T

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4-quinolone derivatives: High-affinity ligands at the benzodiazepine site of brain GABA(A) receptors. synthesis, pharmacology, and pharmacophore modeling

机译：4-喹诺酮衍生物：大脑GABA（A）受体的苯二氮卓部位的高亲和力配体。合成，药理学和药效团建模

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The 3-ethoxycarbonyl-4-quinolone compound I has previously been identified via a database search as an interesting lead compound for ligand binding at the benzodiazepine site of GABA(A) receptors (Kahnberg et al. J. Mol. Graphics Modelling 2004, 23, 253-261). Pharmacophore-guided optimization of this lead compound yielded a number of high-affinity ligands for the benzodiazepine site including compounds 20 and 23-25 displaying sub-nanomolar affinities. A few of the compounds have been tested on the alpha(1)beta(2)gamma(2s) and alpha(3)beta(2)gamma(2s) GABA(A) receptor subtypes, and two of the compounds (5 and 19) display selectivity for alpha(1) versus alpha(3)-containing receptors by a factor of 22 and 27, respectively. This selectivity for alpha(1)beta(2)gamma(2s) is in the same range as that for the well-known alpha(1) subunit selective compound zolpidem.

机译：先前已通过数据库搜索将3-乙氧基羰基-4-喹诺酮化合物I鉴定为在GABA（A）受体的苯并二氮杂位上结合配体的有趣先导化合物（Kahnberg等人，J。Mol。Graphics Modeling 2004，23 ，253-261）。该前导化合物的药理学指导优化产生了苯并二氮杂dia位点的许多高亲和力配体，包括显示出亚纳摩尔亲和力的化合物20和23-25。其中一些化合物已针对alpha（1）beta（2）gamma（2s）和alpha（3）beta（2）gamma（2s）GABA（A）受体亚型进行了测试，其中两种化合物（5和19）显示对含alpha（1）的受体与含alpha（3）的受体的选择性分别为22和27倍。对alpha（1）beta（2）gamma（2s）的选择性与众所周知的alpha（1）亚基选择性化合物唑吡坦的选择性相同。

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《Journal of Medicinal Chemistry》 |2006年第8期|共8页
作者
Lager E; Andersson P; Nilsson J; Pettersson I; Nielsen EO; Nielsen M; Sterner O; Liljefors T;
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正文语种 eng
中图分类药学;
关键词
MOLECULAR MECHANICS; SUBTYPES; BINDING; SOLVATION;

机译：分子力学;亚型;结合;求解;

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1. 4-quinolone derivatives: High-affinity ligands at the benzodiazepine site of brain GABA(A) receptors. synthesis, pharmacology, and pharmacophore modeling [J] . Lager E, Andersson P, Nilsson J, Journal of Medicinal Chemistry . 2006,第8期

机译：4-喹诺酮衍生物：大脑GABA（A）受体的苯二氮卓部位的高亲和力配体。合成，药理学和药效团建模
2. 3D-QSAR studies of 4-quinolone derivatives as high-affinity ligands at the benzodiazepine site of brain GABA_A receptors [J] . Medicinal Chemistry Research . 2011,第2期

机译：3D-QSAR研究脑GABA _{A 受体的苯并二氮杂位上作为高亲和力配体的4-喹诺酮衍生物}
3. 3D-QSAR studies of 4-quinolone derivatives as high-affinity ligands at the benzodiazepine site of brain GABA_A receptors [J] . Anand Gaurav, Mange R. Yadav, Rajani Giridhar, Medicinal chemistry research: an international journal for rapid communications on design and mechanisms of action of biologically active agents . 2011,第2期

机译：3D-QSAR研究脑中GABA_A受体的苯并二氮杂位上作为高亲和力配体的4-喹诺酮衍生物
4. Indentification of Pharmacophore Model, Synthesis and biological evaluation of N-phenyl-1-arylamide and N-phenylbenzenesulfonamide derivatives as BACE 1 inhibitors [C] . Wenhai Huang, Haiping Yu, Rong Sheng, 第四届国际分子模拟与信息技术应用学术会议（The 4th International Conference of Molecular Simulations and Applied Informatics Technologies）论文集 . 2008

机译：N-苯基-1-芳酰胺和N-苯基苯磺酰胺衍生物作为BACE 1抑制剂的药理模型鉴定，合成及生物学评价
5. Part One. Synthesis of optically active tryptophan derivatives with potential activity as indoleamine 2,3-dioxygenase inhibitors: An approach via asymmetric catalytic hydrogenation. Part Two. Design, synthesis and pharmacology of selective ligands for alpha1-containing GABA(A)/benzodiazepine receptor subtypes: SAR studies of beta-carbolines at positions -3 and -6 and their corresponding bivalent ligands. Part Three. First enantiospecific total synthesis of the important biogenetic intermediates, (+)-polyneuridine and (+)-polyneuridine aldehyde, as well as 16-epi-vellosimine and macusine A. [D] . Yin, Wenyuan. 2007

机译：第一部分。具有吲哚胺2,3-二加氧酶抑制剂潜在活性的旋光色氨酸衍生物的合成：一种通过不对称催化氢化的方法。第二部分。含α1的GABA（A）/苯并二氮杂receptor受体亚型的选择性配体的设计，合成和药理作用：位于-3和-6位的β-咔啉及其相应的二价配体的SAR研究。第三部分。重要生物遗传中间体，（+）-聚神经氨酸和（+）-聚神经氨酸醛，以及16-表-维西辛和Macusine A的首次对映体全合成。
6. Interaction of beta-carboline inverse agonists for the benzodiazepine site with another site on GABAA receptors. [O] . H K Im, W B Im, D B Carter, 1995

机译：β-咔啉反向激动剂对苯并二氮杂site位点与GABAA受体上另一个位点的相互作用。
7. HZ166, a novel GABAA receptor subtype-selective benzodiazepine site ligand, is antihyperalgesic in mouse models of inflammatory and neuropathic pain [O] . Di Lio, Alessandra, Benke, Dietmar, Besson, Marie, 2011

机译：HZ166是一种新型的GABAA受体亚型选择性苯二氮卓类位点配体，在炎症性和神经性疼痛的小鼠模型中具有镇痛作用

4-quinolone derivatives: High-affinity ligands at the benzodiazepine site of brain GABA(A) receptors. synthesis, pharmacology, and pharmacophore modeling

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