High end GPCR design: crafted ligand design and druggability analysis using protein structure, lipophilic hotspots and explicit water networks

Jonathan S Mason; Andrea Bortolato; Dahlia R Weiss; Francesca Deflorian; Benjamin Tehan; Fiona H Marshall

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High end GPCR design: crafted ligand design and druggability analysis using protein structure, lipophilic hotspots and explicit water networks

机译：高端GPCR设计：利用蛋白质结构，亲脂性热点和明确的水网络进行精心设计的配体设计和可药性分析

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摘要

Purpose G Protein-Coupled Receptors (GPCRs) are a large family of therapeutically important proteins and as diverse X-ray structures become available it is increasingly possible to leverage structural information for rational drug design.

机译：目的G蛋白偶联受体（GPCR）是重要的治疗蛋白家族，随着各种X射线结构的出现，越来越有可能利用结构信息进行合理的药物设计。

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来源
《In Silico Pharmacology》 |2013年第1期|1-12|共12页
作者
Jonathan S Mason; Andrea Bortolato; Dahlia R Weiss; Francesca Deflorian; Benjamin Tehan; Fiona H Marshall;
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正文语种 eng
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关键词
GPCR; StaR; GRID; WaterMap; WaterFLAP; metadynamics; A2A;

机译：GPCR;星;GRID;水地图;WaterFLAP;元动力学A2A;

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专利

1. High end GPCR design: crafted ligand design and druggability analysis using protein structure, lipophilic hotspots and explicit water networks [J] . Jonathan S Mason, Andrea Bortolato, Dahlia R Weiss, In Silico Pharmacology . 2013,第1期

机译：高端GPCR设计：利用蛋白质结构，亲脂性热点和明确的水网络进行精心设计的配体设计和可药性分析
2. Exploring G Protein-Coupled Receptors (GPCRs) Ligand Space via Cheminformatics Approaches: Impact on Rational Drug Design [J] . Shaherin Basith, Minghua Cui, Stephani J. Y. Macalino, Frontiers in Pharmacology . 2018,第8期

机译：通过化学信息学方法探索G蛋白偶联受体（GPCR）配体空间：对合理药物设计的影响
3. Exploring G Protein-Coupled Receptors (GPCRs) Ligand Space via Cheminformatics Approaches: Impact on Rational Drug Design [J] . Shaherin Basith, Minghua Cui, Stephani J. Y. Macalino, Frontiers in Pharmacology . 2018,第2012期

机译：通过化学信息学方法探索G蛋白偶联受体（GPCR）配体空间：对合理药物设计的影响
4. PREDICTION OF STRUCTURE OF G-PROTEIN COUPLED RECEPTORS AND OF BOUND LIGANDS, WITH APPLICATIONS FOR DRUG DESIGN [C] . YOUYONG LI, WILLIAM A. GODDARD III Pacific Symposium on Biocomputing; 20080104-08; Kohala Coast,HI(US) . 2008

机译：G蛋白偶联受体和结合配体的结构预测及其在药物设计中的应用
5. Studies in structure-based drug design: Ligand design with a flexible protein. [D] . Stultz, Collin Melveton. 1997

机译：基于结构的药物设计研究：具有柔性蛋白质的配体设计。
6. High end GPCR design: crafted ligand design and druggability analysis using protein structure lipophilic hotspots and explicit water networks [O] . Jonathan S Mason, Andrea Bortolato, Dahlia R Weiss, 2013

机译：高端GPCR设计：利用蛋白质结构亲脂性热点和明确的水网络进行精心设计的配体设计和可药性分析
7. High end GPCR design: crafted ligand design and druggability analysis using protein structure, lipophilic hotspots and explicit water networks [O] . Jonathan S Mason, Andrea Bortolato, Dahlia R Weiss, 2013

机译：高端GPCR设计：利用蛋白质结构，亲脂性热点和明确的水网络进行精心设计的配体设计和可药性分析

High end GPCR design: crafted ligand design and druggability analysis using protein structure, lipophilic hotspots and explicit water networks

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