共 60 条
GPCR activation: a mutagenic spotlight on crystal structures
被引:57
作者:

Hulme, Edward C.
论文数: 0 引用数: 0
h-index: 0
机构:
MRC Natl Inst Med Res, Div Phys Biochem, London NW7 1AA, England MRC Natl Inst Med Res, Div Phys Biochem, London NW7 1AA, England
机构:
[1] MRC Natl Inst Med Res, Div Phys Biochem, London NW7 1AA, England
基金:
英国医学研究理事会;
关键词:
MUSCARINIC ACETYLCHOLINE-RECEPTOR;
PROTEIN-COUPLED RECEPTORS;
TRANSMEMBRANE DOMAIN;
CONSTITUTIVE ACTIVATION;
CONFORMATIONAL-CHANGES;
ALLOSTERIC MODULATION;
SCANNING MUTAGENESIS;
EXTRACELLULAR LOOP;
FUNCTIONAL-ROLE;
HELIX MOVEMENT;
D O I:
10.1016/j.tips.2012.11.002
中图分类号:
R9 [药学];
学科分类号:
1007 ;
摘要:
The crystal structures of antagonist and agonist complexes of isolated beta(2) and beta(1) adrenoceptors have recently been supplemented by antagonist structures of M-2 and M-3 muscarinic acetylcholine receptors. Importantly, a structure of an agonist-ligated beta(2) adrenoceptor complexed with its cognate G protein has provided the first view of a ternary complex representing the transition state in agonist-mediated G protein activation. This review interprets these G-protein-coupled receptor (GPCR) structures through the focus provided by extensive mutagenesis studies on muscarinic receptors, revealing an activation mechanism that is both modular and dynamic. Specific motifs, based around highly conserved residues, functionalise the seven-transmembrane architecture of these receptors. While exploiting conserved motifs, the ligand binding and signal transduction pathways work around and through water-containing cavities, an emerging feature of GPCR structures. These cavities may have undergone evolutionary selection to adapt GPCRs to particular signalling niches, and may provide targeting opportunities to enhance drug selectivity.
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页码:67 / 84
页数:18
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