G-蛋白偶联受体GPR120分子模建研究  被引量:4

G-Protein-Coupled Receptor 120-GPR120:Molecular Modeling Studies

在线阅读下载全文

作  者:陆绍永[1] 蒋勇军[2] 俞庆森[1] 邹建卫[2] 

机构地区:[1]浙江大学化学系,杭州310027 [2]浙江大学宁波理工学院分子设计与营养工程市重点实验室,宁波315104

出  处:《化学学报》2009年第14期1553-1558,共6页Acta Chimica Sinica

基  金:国家863项目(No.2007AA02Z301);国家自然科学基金(No.20803063)资助项目

摘  要:新的长链脂肪酸受体G-蛋白偶联受体120(G-protein-coupled receptor120,GPR120)是2型糖尿病的潜在治疗靶标.由于其晶体结构迄今尚未获得,成为基于结构的新药设计的瓶颈.首先,以人体β2肾上腺能素受体(human β2 adrenergic receptor,β2AR)晶体结构为模板,通过同源模建方法构建GPR120三维结构,对整个体系进行包膜的分子动力学模拟.然后采用分子对接技术模建了GPR120的小分子激动剂GW9508与GPR120的相互作用模型,发现了受体分子识别的关键性残基,为开展定点突变实验提供了指导意义.所建模型为研究受体与配体作用提供了合理的初始结构,此方法也适用于其他G蛋白偶联受体的分子模建.G-protein-coupled receptor 120 (GPR 120), which functions as a new receptor for long chain free fatty acids, may play a role as a potential therapeutic target for type 2 diabetes mellitus. The three-dimensional (3D) structure of GPR120 is experimentally unavailable to date, however, leading to difficulty in the structure-based drug design. Based on the X-ray crystal structure of f12 adrenergic receptor, a homology model of the GPR120 was constructed, then, molecular-dynamics (MD) simulations were carried out for the entire system. The GPR120 ligand agonist GW9508 was docked into the optimized model, and the critical amino acid residues for binding were identified, which was very important for further site-directed mutagenesis study. The constructed models should provide a good starting point for further characterization of the binding models for GPR120 ligands. Furthermore, the method developed herein will be applicable to build other GPCRs.

关 键 词:G-蛋白偶联受体 GPR120 同源模建 分子动力学模拟 2型糖尿病 

分 类 号:O629.7[理学—有机化学]

 

参考文献:

正在载入数据...

 

二级参考文献:

正在载入数据...

 

耦合文献:

正在载入数据...

 

引证文献:

正在载入数据...

 

二级引证文献:

正在载入数据...

 

同被引文献:

正在载入数据...

 

相关期刊文献:

正在载入数据...

相关的主题
相关的作者对象
相关的机构对象