Molecular mechanism of GPCR spatial organization at the plasma membrane.
Gabriele KockelkorenLine LauritsenChristopher G ShuttleEleftheria KazepidouIvana VonkovaYunxiao ZhangArtú BreuerCeleste KennardRachel M BrunettiElisa D'EsteOrion David WeinerMark UlineDimitrios StamouPublished in: Nature chemical biology (2023)
G-protein-coupled receptors (GPCRs) mediate many critical physiological processes. Their spatial organization in plasma membrane (PM) domains is believed to encode signaling specificity and efficiency. However, the existence of domains and, crucially, the mechanism of formation of such putative domains remain elusive. Here, live-cell imaging (corrected for topography-induced imaging artifacts) conclusively established the existence of PM domains for GPCRs. Paradoxically, energetic coupling to extremely shallow PM curvature (<1 µm -1 ) emerged as the dominant, necessary and sufficient molecular mechanism of GPCR spatiotemporal organization. Experiments with different GPCRs, H-Ras, Piezo1 and epidermal growth factor receptor, suggest that the mechanism is general, yet protein specific, and can be regulated by ligands. These findings delineate a new spatiomechanical molecular mechanism that can transduce to domain-based signaling any mechanical or chemical stimulus that affects the morphology of the PM and suggest innovative therapeutic strategies targeting cellular shape.
Keyphrases
- particulate matter
- air pollution
- epidermal growth factor receptor
- polycyclic aromatic hydrocarbons
- heavy metals
- high resolution
- water soluble
- tyrosine kinase
- advanced non small cell lung cancer
- oxidative stress
- diabetic rats
- high glucose
- drug delivery
- drug induced
- risk assessment
- cancer therapy
- fluorescence imaging
- protein protein
- mass spectrometry
- stress induced
- small molecule
- amino acid
- ionic liquid
- drug discovery
- structural basis