Synthesis and structure-affinity relationships of 1,3, 5-alkylsubstituted cyclohexylamines binding at NMDA receptor PCP site.

Jirgensons A; Kauss V; Kalvinsh I; Gold MR; Danysz W; Parsons CG; Quack G

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Synthesis and structure-affinity relationships of 1,3, 5-alkylsubstituted cyclohexylamines binding at NMDA receptor PCP site.

机译：在NMDA受体PCP位点结合的1,3,5-烷基取代的环己胺的合成与结构亲和关系。

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摘要

A series of 1,3,5-alkylsubstituted cyclohexylamines 2 were synthesized as ligands for the N-methyl-D-aspartate (NMDA) receptor phencyclidine (PCP) binding site. Pure diastereomers with defined configuration of amino group 2-ax and 2-eq were obtained. The optimal size of 1,3,5-substituents was determined for cyclohexylamines 2 with an equatorial amino group in the lowest energy conformation using Hansch analysis. According to the data, the lipophilic part of cyclohexylamines 2 does not discriminate between hydrophobic regions of the PCP binding site but rather recognizes this site as a whole lipophilic pocket.

机译：合成了一系列的1,3,5-烷基取代的环己胺2作为N-甲基-D-天冬氨酸（NMDA）受体苯环利定（PCP）结合位点的配体。获得具有2-氨基和2-eq氨基的确定构型的纯非对映异构体。使用Hansch分析，以最低能量构象确定具有赤道氨基的环己胺2的1,3,5-取代基的最佳尺寸。根据数据，环己胺2的亲脂性部分不能区分PCP结合位点的疏水区域，而是将该位点识别为整个亲脂性口袋。

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来源
《European Journal of Medicinal Chemistry: Chimie Therapeutique》 |2000年第6期|共11页
作者
Jirgensons A; Kauss V; Kalvinsh I; Gold MR; Danysz W; Parsons CG; Quack G;
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原文格式 PDF
正文语种 eng
中图分类医药、卫生;
关键词
Cyclohexylamines; Phencyclidine; Receptors; N-Methyl-D-Aspartate; Amantadine; 环己胺类; 苯环利定; 受体; N-甲基-D-天冬氨酸;

机译：Cyclohexylamines;Phencyclidine;Receptors;N-Methyl-D-Aspartate;Amantadine;环己胺类;苯环利定;受体;N-甲基-D-天冬氨酸;

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1. Synthesis and structure-affinity relationships of 1,3, 5-alkylsubstituted cyclohexylamines binding at NMDA receptor PCP site. [J] . Jirgensons A, Kauss V, Kalvinsh I, European Journal of Medicinal Chemistry: Chimie Therapeutique . 2000,第6期

机译：在NMDA受体PCP位点结合的1,3,5-烷基取代的环己胺的合成与结构亲和关系。
2. 1,3-dialkyl-8-N-substituted benzyloxycarbonylamino-9-deazaxanthines as potent adenosine receptor ligands: Design, synthesis, structure-affinity and structure-selectivity relationships. [J] . Fernandez F, Caamano O, Isabel Nieto M Bioorganic and medicinal chemistry . 2009,第10期

机译：1,3-二烷基-8-N-取代的苄氧基羰基氨基-9-脱氮黄嘌呤作为有效的腺苷受体配体：设计，合成，结构亲和力和结构选择性关系。
3. 1,3-Dialkyl-8-(hetero)aryl-9-OH-9-deazaxanthines as potent A_(2B) adenosine receptor antagonists: design, synthesis, structure-affinity and structure-selectivity relationships. [J] . Stefanachi A, Nicolotti O, Leonetti F, Bioorganic and medicinal chemistry . 2008,第22期

机译：1,3-二烷基-8-（杂）芳基-9-OH-9-脱黄嘌呤类作为有效的A_（2B）腺苷受体拮抗剂：设计，合成，结构亲和力和结构选择性关系。
4. Mass Spectrometry of the Interaction Between Calmodulin and ER(alpha)17p, a Peptide That Corresponds to the Estrogen Receptor/Calmodulin-Binding Site. [C] . Sandrine Voillard, Francoise Fournier, Carlos Afonso, American Society for Mass Spectrometry Conference on Mass Spectrometry and Allied Topics . 2009

机译：钙调蛋白和ER（α）17p的相互作用的质谱，肽与雌激素受体/钙调蛋白结合位点对应的肽。
5. Differential effect of metaphit on the biochemical and functional properties of receptors for N-methyl-D-aspartate (NMDA) and phencyclidine (PCP). [D] . Wyatt, Lindy McNabb. 1991

机译：隐喻对N-甲基-D-天冬氨酸（NMDA）和苯环利定（PCP）受体的生化和功能特性的差异作用。
6. Synthesis Structure-Affinity Relationships and Modeling of AMDA Analogs at 5-HT2A and H1 Receptors: Structural Factors Contributing to Selectivity [O] . Jitesh R. Shah, Philip D. Mosier, Bryan L. Roth, -1

机译：5-HT2A和H1受体中AMDA类似物的合成结构 - 亲和力关系和模拟：有助于选择性的结构因素
7. Fluorine-Substituted Cyclofenil Derivatives as Estrogen Receptor Ligands: Synthesis and Structure-Affinity Relationship Study of Potential Positron Emission Tomography Agents for Imaging Estrogen Receptors in Breast Cancer [O] . -1

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8. Structure-Affinity Study of the Binding of 4-Substituted Analogues of 1-(2,5-Dimethoxyphenyl)-2-Aminopropane at 5-HT(2) Serotonin Receptors [R] . Seggel, M. R., Yousif, M. Y., Lyon, R. A., 1990

机译：4-（2,5-二甲氧基苯基）-2-氨基丙烷的4-取代类似物在5-HT（2）5-羟色胺受体上的结合亲和性研究

Synthesis and structure-affinity relationships of 1,3, 5-alkylsubstituted cyclohexylamines binding at NMDA receptor PCP site.

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