Recent Trends and Applications of Molecular Modeling in GPCR–Ligand Recognition and Structure-Based Drug Design

机译：分子模型在GPCR中的最新趋势和应用-配体识别和基于结构的药物设计

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G protein-coupled receptors represent the largest family of human membrane proteins and are modulated by a variety of drugs and endogenous ligands. Molecular modeling techniques, especially enhanced sampling methods, have provided significant insight into the mechanism of GPCR–ligand recognition. Notably, the crucial role of the membrane in the ligand-receptor association process has earned much attention. Additionally, docking, together with more accurate free energy calculation methods, is playing an important role in the design of novel compounds targeting GPCRs. Here, we summarize the recent progress in the computational studies focusing on the above issues. In the future, with continuous improvement in both computational hardware and algorithms, molecular modeling would serve as an indispensable tool in a wider scope of the research concerning GPCR–ligand recognition as well as drug design targeting GPCRs.

机译：G蛋白偶联受体代表人类膜蛋白的最大家族，并受多种药物和内源性配体的调节。分子建模技术，尤其是增强的采样方法，已经为GPCR-配体识别的机理提供了重要的见识。值得注意的是，膜在配体-受体缔合过程中的关键作用已引起广泛关注。此外，对接以及更精确的自由能计算方法在靶向GPCR的新型化合物的设计中起着重要作用。在这里，我们总结了针对上述问题的计算机研究的最新进展。将来，随着计算硬件和算法的不断改进，分子模型将成为有关GPCR-配体识别以及针对GPCR的药物设计的更广泛研究中必不可少的工具。

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期刊名称 International Journal of Molecular Sciences
作者
Xiaojing Yuan; Yechun Xu;
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作者单位

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年(卷),期 2018(19),7
年度 2018
页码 2105
总页数 16
原文格式 PDF
正文语种
中图分类分子生物学;
关键词
GPCR receptor–ligand recognition drug design molecular modeling molecular dynamics docking binding affinity binding pathway;

机译：GPCR;受体-配体识别;药物设计;分子模型;分子动力学;对接;结合亲和力;结合途径;

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专利

1. New Trends in Inspecting GPCR‐ligand Recognition Process: the Contribution of the Molecular Modeling Section (MMS) at the University of Padova [J] . Ciancetta Antonella, Cuzzolin Alberto, Deganutti Giuseppe, Molecular informatics . 2016,第8a9期

机译：检查GPCR-Ligand识别过程的新趋势：分子建模部分（MMS）在帕多瓦大学的贡献
2. Class A GPCRs: Structure, Function, Modeling and Structure-based Ligand Design [J] . Xiaojing Cong, Jeremie Topin Jerome Golebiowski Current pharmaceutical design . 2017,第29期

机译：A类GPCR：结构，功能，建模和结构的配体设计
3. Structure-based drug design using GPCR homology modeling: Toward the discovery of novel selective CysLT2 antagonists [J] . DongX., ZhaoY., HuangX., European Journal of Medicinal Chemistry: Chimie Therapeutique . 2013,第Null期

机译：使用GPCR同源性建模的基于结构的药物设计：寻求新型选择性CysLT2拮抗剂的发现
4. A new molecular simulation software package-Peking University Drug Design System (PKUDDS) for structure-based drug design [C] . 北京大学中医药现代研究中心2001年年会论文集 . 2000

机译：一种新的分子模拟软件包-北京大学药物设计系统（PKUDDS），用于基于结构的药物设计
5. Computational simulations of protein-ligand molecular recognition via enhanced samplings, free energy calculations and applications to structure-based drug design. [D] . Park, In-Hee. 2010

机译：蛋白质-配体分子识别的计算模拟，包括增强采样，自由能计算以及在基于结构的药物设计中的应用。
6. Challenges Applications and Recent Advances of Protein-Ligand Docking in Structure-Based Drug Design [O] . Sam Z. Grinter, Xiaoqin Zou 2014

机译：蛋白质-配体对接在基于结构的药物设计中的挑战应用和最新进展
7. Challenges, Applications, and Recent Advances of Protein-Ligand Docking in Structure-Based Drug Design [O] . Sam Z. Grinter, Xiaoqin Zou 2014

机译：基于结构的药物设计中蛋白质 - 配体对接的挑战，应用和最新进展

Recent Trends and Applications of Molecular Modeling in GPCR–Ligand Recognition and Structure-Based Drug Design

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