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Predicted structure of fully activated human bitter taste receptor TAS2R4 complexed with G protein and agonists
Predicted structure of fully activated human bitter taste receptor TAS2R4 complexed with G protein and agonists
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Predicted structure of fully activated human bitter taste receptor TAS2R4 complexed with G protein and agonists
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Predicted structure of fully activated human bitter taste receptor TAS2R4 complexed with G protein and agonists
Predicted structure of fully activated human bitter taste receptor TAS2R4 complexed with G protein and agonists

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Predicted structure of fully activated human bitter taste receptor TAS2R4 complexed with G protein and agonists
Predicted structure of fully activated human bitter taste receptor TAS2R4 complexed with G protein and agonists
Journal Article

Predicted structure of fully activated human bitter taste receptor TAS2R4 complexed with G protein and agonists

2021
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Overview
Bitter taste is sensed by bitter taste receptors (TAS2Rs) that belong to the G protein-coupled receptor (GPCR) superfamily. In addition to bitter taste perception, TAS2Rs have been reported recently to be expressed in many extraoral tissues and are now known to be involved in health and disease. Despite important roles of TAS2Rs in biological functions and diseases, no crystal structure is available to help understand the signal transduction mechanism or to help develop selective ligands as new therapeutic targets. We report here the three-dimensional structure of the fully activated TAS2R4 human bitter taste receptor predicted using the GEnSeMBLE complete sampling method. This TAS2R4 structure is coupled to the gustducin G protein and to each of several agonists. We find that the G protein couples to TAS2R4 by forming strong salt bridges to each of the three intracellular loops, orienting the activated Gα5 helix of the Gα subunit to interact extensively with the cytoplasmic region of the activated receptor. We find that the TAS2Rs exhibit unique motifs distinct from typical Class A GPCRs, leading to a distinct activation mechanism and a less stable inactive state. This fully activated bitter taste receptor complex structure provides insight into the signal transduction mechanism and into ligand binding to TAS2Rs.