Structural biology of insulin and IGF1 receptors: implications for drug design

被引:0
作者
Pierre De Meyts
Jonathan Whittaker
机构
[1] Receptor Biology Laboratory,
[2] Hagedorn Research Institute,undefined
来源
Nature Reviews Drug Discovery | 2002年 / 1卷
关键词
D O I
暂无
中图分类号
学科分类号
摘要
The cloning of the complementary DNAs and genes for the insulin and insulin-like growth factor 1 (IGF1) receptors, as well as tertiary-structure predictions, have provided valuable insights into the overall domain organization of the receptors.No crystal structure of the insulin- or IGF1-receptor complexes with their ligands is yet available, but crystal structures of the large domain 1 (L1)–Cys-rich (CR)–L2 amino-terminal fragment of the IGF1 receptor, and of the insulin- and IFG1-receptor tyrosine-kinase domains both in the inactive and activated conformation, are available.Single-molecule electron-microscopic imaging of the insulin receptor has given some indications of the overall organization of the extracellular receptor domains, although there have been variable results and a tendency in some cases to over-interpret low-resolution data.Knowledge of the structure of several receptor tyrosine-kinase domains has led to attempts to screen for, or design, mimetics or inhibitors, with some degree of success. Agonists or antagonists that target the ligand-binding sites might have a greater chance to be selective, hence the importance of understanding the nature of the ligand-binding mechanism.Mapping the ligand-binding sites on the insulin and IGF1 receptors by receptor crosslinking with photoreactve ligands, by examining the binding selectivity of chimeric insulin–IGF1 receptors, by alanine-scanning mutagenesis of receptor domains and by reconstitution of minimized receptor constructs with low or high affinity, has provided a wealth of information on the binding epitopes.Likewise, mapping of the residues on the insulin molecule that are involved in receptor binding has progressed, and has revealed the existence of a second binding surface in addition to the so-called 'classical' binding surface. The information on IGF1 and IGF2 is more fragmentary.Alternative crosslinking models that explain the complex ligand-binding kinetics of the insulin and IGF1 receptors (including negative cooperativity) are discussed.Various strategies for designing agonists or antagonists of a dimerizing receptor are discussed, building on the experience acquired with the erythropoietin receptor.
引用
收藏
页码:769 / 783
页数:14
相关论文
共 337 条
[21]  
Whittaker J(1995)Insulin and epidermal growth factor receptors contain the cysteine repeat motif found in the tumor necrosis factor receptor Proteins 22 141-153
[22]  
Ullrich A(1998)A third fibronectin type III domain in the extracellular region of the insulin receptor family FEBS Lett. 441 331-336
[23]  
Seino S(1998)A third fibronectin-type-III domain in the insulin-family receptors Trends Biol. Sci. 23 465-466
[24]  
Seino M(1999)Members of the insulin receptor family contain three fibronectin type III domains Growth Factors 16 315-322
[25]  
Nishi S(1998)Crystal structure of the first three domains of the type-1 insulin-like growth factor receptor Nature 394 395-399
[26]  
Bell GI(1998)Expression and characterization of a 70-kDa fragment of the insulin receptor that binds insulin. Minimizing ligand binding domain of the insulin receptor J. Biol. Chem. 273 17780-17786
[27]  
Abbott AM(2000)Structural domains of the insulin receptor and IGF receptor required for dimerisation and ligand binding FEBS Lett. 467 226-230
[28]  
Bueno R(1994)Crystal structure of the tyrosine kinase domain of the human insulin receptor Nature 372 746-754
[29]  
Pedrini MT(1997)Crystal structure of the activated insulin receptor tyrosine kinase in complex with peptide substrate and ATP analog EMBO J. 16 5572-5581
[30]  
Murray JM(2001)Structure and autoregulation of the insulin-like growth factor 1 receptor kinase Nature Struct. Biol. 8 1058-1063
12345678910