Structural basis for signal recognition and transduction by platelet-activating-factor receptor.
Can CaoQiuxiang TanChanjuan XuLingli HeLinlin YangYe ZhouYiwei ZhouAnna QiaoMinmin LuCuiying YiGye Won HanXianping WangXuemei LiHuaiyu YangZihe RaoHualiang JiangYongfang ZhaoJianfeng LiuRaymond C StevensQiang ZhaoXuejun C ZhangBeili WuPublished in: Nature structural & molecular biology (2018)
Platelet-activating-factor receptor (PAFR) responds to platelet-activating factor (PAF), a phospholipid mediator of cell-to-cell communication that exhibits diverse physiological effects. PAFR is considered an important drug target for treating asthma, inflammation and cardiovascular diseases. Here we report crystal structures of human PAFR in complex with the antagonist SR 27417 and the inverse agonist ABT-491 at 2.8-Å and 2.9-Å resolution, respectively. The structures, supported by molecular docking of PAF, provide insights into the signal-recognition mechanisms of PAFR. The PAFR-SR 27417 structure reveals an unusual conformation showing that the intracellular tips of helices II and IV shift outward by 13 Å and 4 Å, respectively, and helix VIII adopts an inward conformation. The PAFR structures, combined with single-molecule FRET and cell-based functional assays, suggest that the conformational change in the helical bundle is ligand dependent and plays a critical role in PAFR activation, thus greatly extending knowledge about signaling by G-protein-coupled receptors.
Keyphrases
- single molecule
- molecular docking
- molecular dynamics simulations
- single cell
- cell therapy
- cardiovascular disease
- signaling pathway
- atomic force microscopy
- healthcare
- living cells
- endothelial cells
- oxidative stress
- structural basis
- emergency department
- chronic obstructive pulmonary disease
- stem cells
- high throughput
- bone marrow
- cardiovascular events
- allergic rhinitis