Validated ligand binding sites in CCK receptors. next step: computer-aided design of novel CCK ligands.

Tikhonova IG; Marco E; Lahlou-Archer E; Langer I; Foucaud M; Maigret B; Fourmy D

首页> 外文期刊>Current topics in medicinal chemistry >Validated ligand binding sites in CCK receptors. next step: computer-aided design of novel CCK ligands.

【24h】

Validated ligand binding sites in CCK receptors. next step: computer-aided design of novel CCK ligands.

机译：验证了CCK受体中的配体结合位点。下一步：新型CCK配体的计算机辅助设计。

获取原文

获取原文并翻译 | 示例

掌桥外文数据库（机构版） >>

开具论文收录证明 >>

文献代查 >>

页面导航

摘要
著录项
相似文献
相关主题

摘要

Computer-aided drug design becomes an important part of G-protein coupled receptors (GPCR) drug discovery process that is applied for improving the efficiency of derivation and optimization of novel ligands. It represents the combination of methods that use structural information of a receptor binding site of known ligands to design new ligands. In this report, we give a brief description of ligand binding sites in cholecystokinin and gastrin receptors (CCK1R and CCK2R) which were delineated using experimental and computational methods, and then, we show how the validated ligand binding sites can be used to design and improve novel ligands. The translation of the knowledge of ligand-binding sites of different GPCRs to computer-aided design of novel ligands is summarized.

机译：计算机辅助药物设计成为G蛋白偶联受体（GPCR）药物发现过程的重要组成部分，该过程可用于提高衍生效率和优化新型配体。它代表了使用已知配体受体结合位点的结构信息设计新配体的方法的组合。在本报告中，我们简要介绍了胆囊收缩素和胃泌素受体（CCK1R和CCK2R）中的配体结合位点，并使用实验和计算方法对其进行了描述，然后，我们展示了如何将经过验证的配体结合位点用于设计和改进新的配体。总结了将不同GPCR的配体结合位点的知识翻译为新型配体的计算机辅助设计的过程。

著录项

来源
《Current topics in medicinal chemistry》 |2007年第12期|共5页
作者
Tikhonova IG; Marco E; Lahlou-Archer E; Langer I; Foucaud M; Maigret B; Fourmy D;
展开▼
作者单位

展开▼
收录信息
原文格式 PDF
正文语种 eng
中图分类药学;
关键词
novel; Ligands; Cholecystokinin; Binding Sites; 配体; 缩胆囊素; 结合部位;

机译：novel;Ligands;Cholecystokinin;Binding Sites;配体;缩胆囊素;结合部位;

相似文献

外文文献
中文文献
专利

1. Validated ligand binding sites in CCK receptors. next step: computer-aided design of novel CCK ligands. [J] . Tikhonova IG, Marco E, Lahlou-Archer E, Current topics in medicinal chemistry . 2007,第12期

机译：验证了CCK受体中的配体结合位点。下一步：新型CCK配体的计算机辅助设计。
2. How a single inversion of configuration leads to a reversal of the binding mode: proposal of a novel arrangement of CCK2 ligands in their receptor, and contribution to the development of peptidomimetic or non-peptide CCK2 ligands. [J] . Bellier B, Garbay C European Journal of Medicinal Chemistry: Chimie Therapeutique . 2003,第7a8期

机译：构型的一次反转如何导致结合模式的逆转：CCK2配体在其受体中的新型排列的提议，以及对拟肽或非肽CCK2配体的发展的贡献。
3. Strategies for design of non peptide CCK1R agonist/antagonist ligands. [J] . Garcia-Lopez MT, Gonzalez-Muniz R, Martin-Martinez M, Current topics in medicinal chemistry . 2007,第12期

机译：非肽CCK1R激动剂/拮抗剂配体的设计策略。
4. Design and synthesis of bifunctional peptides:antagonists at CCKA/CCKB receptors and agonists as mu/delta opioid receptors [C] . Richard S.Agnes, Yeon Sun Lee, Peg Davis, the International Peptide Symposium . 2001

机译：双官能肽的设计与合成：Ccka / Cckb受体的拮抗剂和穆/δ阿片受体的激动剂
5. Probing the ligand-binding pocket of the cannabinoid receptors: Design and synthesis of novel ligands. [D] . Krishnamurthy, Mathangi. 2005

机译：探测大麻素受体的配体结合口袋：新型配体的设计和合成。
6. Trigeminal and dorsal root ganglion neurons express CCK receptor binding sites in the rat rabbit and monkey: possible site of opiate- CCK analgesic interactions [O] . JR Ghilardi, CJ Allen, SR Vigna, 1992

机译：三叉神经和背根神经节神经元在大鼠兔子和猴子中表达CCK受体结合位点：鸦片-CCK镇痛作用的可能位点
7. The cholecystokinin analogues JMV-180 and CCK-8 stimulate phospholipase C through the same binding site of CCKA receptor in rat pancreatic acini [O] . Sarri, Elisabet, Ramos, Belén, Salido, Ginés M, 2001

机译：胆囊收缩素类似物JMV-180和CCK-8通过CCKA受体在大鼠胰腺腺泡中的相同结合位点刺激磷脂酶C

Validated ligand binding sites in CCK receptors. next step: computer-aided design of novel CCK ligands.

摘要

著录项

相似文献

相关主题

期刊订阅