| Literature DB >> 32632293 |
Lisa J Clark1,2, James Krieger3, Alex D White1,4, Vasyl Bondarenko5, Saifei Lei1, Fei Fang1, Ji Young Lee3, Pemra Doruker3, Thore Böttke6, Frederic Jean-Alphonse1, Pei Tang1,3,5, Thomas J Gardella7, Kunhong Xiao1, Ieva Sutkeviciute1, Irene Coin6, Ivet Bahar8, Jean-Pierre Vilardaga9.
Abstract
Peptide ligands of class B G-protein-coupled receptors act via a two-step binding process, but the essential mechanisms that link their extracellular binding to intracellular receptor-arrestin interactions are not fully understood. Using NMR, crosslinking coupled to mass spectrometry, signaling experiments and computational approaches on the parathyroid hormone (PTH) type 1 receptor (PTHR), we show that initial binding of the PTH C-terminal part constrains the conformation of the flexible PTH N-terminal signaling epitope before a second binding event occurs. A 'hot-spot' PTH residue, His9, that inserts into the PTHR transmembrane domain at this second step allosterically engages receptor-arrestin coupling. A conformational change in PTHR intracellular loop 3 permits favorable interactions with β-arrestin's finger loop. These results unveil structural determinants for PTHR-arrestin complex formation and reveal that the two-step binding mechanism proceeds via cooperative fluctuations between ligand and receptor, which extend to other class B G-protein-coupled receptors.Entities:
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Year: 2020 PMID: 32632293 PMCID: PMC7502484 DOI: 10.1038/s41589-020-0567-0
Source DB: PubMed Journal: Nat Chem Biol ISSN: 1552-4450 Impact factor: 15.040