An arginyl in the N-terminus of the V-1a vasopressin receptor is part of the conformational switch controlling activation by agonist

SR Hawtin, VJ Wesley, John Simms, Rosemary Parslow, A Miles, K McEwan, Mary Keen, Mark Wheatley

Research output: Contribution to journalArticle

8 Citations (Scopus)

Abstract

Defining how the agonist-receptor interaction differs from that of the antagonist-receptor and understanding the mechanisms of receptor activation are fundamental issues in cell signalling. The V-1a vasopressin receptor (V1aR) is a member of a family of related G-protein coupled receptors that are activated by neurohypophysial peptide hormones, including vasopressin (AVP). It has recently been reported that an arginyl in the distal N-terminus of the V1aR is critical for binding agonists but not antagonists. To determine specific features required at this locus to support high affinity agonist binding and second messenger generation, Arg46 was substituted by all other 19 encoded amino acids. Our data establish that there is an absolute requirement for arginyl, as none of the [R46X]V1aR mutant constructs supported high affinity agonist binding and all 19 had defective signalling. In contrast, all of the mutant receptors possessed wildtype binding for both peptide and nonpeptide antagonists. The ratio of K-i to EC50, an indicator of efficacy, was increased for all substitutions. Consequently, although [R46X]V1aR constructs have a lower affinity for agonist, once AVP has bound all 19 are more likely than the wildtype V1aR to become activated. Therefore, in the wildtype V1aR, Arg46 constrains the inactive conformation of the receptor. On binding AVP this constraint is alleviated, promoting the transition to active V1aR. Our findings explain why arginyl is conserved at this locus throughout the evolutionary lineage of the neurohypophysial peptide hormone receptor family of G-protein coupled receptors.
Original languageEnglish
Pages (from-to)4681-4688
Number of pages8
JournalEuropean Journal of Biochemistry
Volume270
Issue number23
DOIs
Publication statusPublished - 1 Dec 2003

Keywords

  • ligand binding
  • cell signaling
  • peptide hormone
  • vasopressin
  • GPCR

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