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Autoregulation of GPCR signalling through the third intracellular loop
[摘要] The third intracellular loop (ICL3) of the G protein-coupled receptor (GPCR) fold is important for the signal transduction process downstream of receptor activation1-3. Despite this, the lack of a defined structure of ICL3, combined with its high sequence divergence among GPCRs, complicates characterization of its involvement in receptor signalling(4). Previous studies focusing on the beta 2 adrenergic receptor (beta 2AR) suggest that ICL3 is involved in the structural process of receptor activation and signalling(5-7). Here we derive mechanistic insights into the role of ICL3 in beta 2AR signalling, observing that ICL3 autoregulates receptor activity through a dynamic conformational equilibrium between states that block or expose the receptor's G protein-binding site. We demonstrate the importance of this equilibrium for receptor pharmacology, showing that G protein-mimetic effectors bias the exposed states of ICL3 to allosterically activate the receptor. Our findings additionally reveal that ICL3 tunes signalling specificity by inhibiting receptor coupling to G protein subtypes that weakly couple to the receptor. Despite the sequence diversity of ICL3, we demonstrate that this negative G protein-selection mechanism through ICL3 extends to GPCRs across the superfamily, expanding the range of known mechanisms by which receptors mediate G protein subtype selective signalling. Furthermore, our collective findings suggest ICL3 as an allosteric site for receptor- and signalling pathway-specific ligands.
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[关键词] BETA(2) ADRENERGIC-RECEPTOR;PROTEIN-COUPLED RECEPTORS;CRYSTAL-STRUCTURE;GS-PROTEIN;ACTIVATION;DYNAMICS;DOMAINS;CONFORMATIONS;SELECTIVITY;INHIBITION [时效性] 
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