Understanding Peptide Binding in Class A G Protein-Coupled Receptors

被引:21
|
作者
Tikhonova, Irina G. [1 ]
Gigoux, Veronique [2 ]
Fourmy, Daniel [2 ]
机构
[1] Queens Univ Belfast, Med Biol Ctr, Sch Pharm, 97 Lisburn Rd, Belfast BT9C7BL, Antrim, North Ireland
[2] Univ Toulouse III, INSA, CNRS,Lab Phys & Chim Nanoobjets, UMR5215,INSERM,ERL1226 Receptol & Therapeut Targe, Toulouse, France
基金
英国生物技术与生命科学研究理事会;
关键词
SITE-DIRECTED MUTAGENESIS; THYROTROPIN-RELEASING-HORMONE; TRANSMEMBRANE DOMAIN 3; C-TERMINAL AMIDE; LIGAND-BINDING; NEUROPEPTIDE-Y; HIGH-AFFINITY; AMINO-ACIDS; STRUCTURAL BASIS; MOLECULAR-BASIS;
D O I
10.1124/mol.119.115915
中图分类号
R9 [药学];
学科分类号
1007 ;
摘要
Many physiologic processes are controlled through the activation of G protein-coupled receptors (GPCRs) by regulatory peptides, making peptide GPCRs particularly useful targets for major human diseases such as diabetes and cancer. Peptide GPCRs are also being evaluated as next-generation targets for the development of novel antiparasite agents and insecticides in veterinary medicine and agriculture. Resolution of crystal structures for several peptide GPCRs has advanced our understanding of peptide-receptor interactions and fueled interest in correlating peptide heterogeneity with receptor-binding properties. In this review, the knowledge of recently crystalized peptide-GPCR complexes, previously accumulated peptide structure-activity relationship studies, receptor mutagenesis, and sequence alignment are integrated to better understand peptide binding to the transmembrane cavity of class A GPCRs. Using SAR data, we show that peptide class A GPCRs can be divided into groups with distinct hydrophilic residues. These characteristic residues help explain the preference of a receptor to bind the C- terminal free carboxyl group, the C-terminal amidated group, or the N-terminal ammonium group of peptides.
引用
收藏
页码:550 / 561
页数:12
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