Y Ala scite author profile

Using a three-dimensional model of G protein-coupled receptors (GPCR), we have previously succeeded in docking the neurohypophysial hormone argininevasopressin (AVP) into the Vla receptor. According to this model, the hormone is completely embedded in the transmembrane part of the receptor. Only the side chain of the Arg residue at position 8 projects outside the transmembrane core of the receptor and possibly interacts with a Tyr residue located in the first extracellular loop at position 115. Residue 8 varies in the two natural neurohypophysial hormones, AVP and oxytocin (OT); similarly, different residues are present at position 115 in the different members of the AVP/ OT receptor family. Here we show that Arg8 is crucial for high affinity binding of AVP to the rat Vla receptor. Moreover, when Tyrl15 is replaced by an Asp and a Phe, the amino acids naturally occurring in the V2 and in the OT receptor subtypes, the agonist selectivity of the Vla receptor switches accordingly. Our results indicate that the interaction between peptide residue 8 and the receptor residue at position 115 is not only crucial for agonist high affinity binding but also for receptor selectivity.

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Properties of a new radioiodinated antagonist for human vasopressin V2 and V1a receptors

Ala

Morin

Mahé

et al. 1997

European Journal of Pharmacology

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Functional studies of twelve mutant V2 vasopressin receptors related to nephrogenic diabetes insipidus

Ala

Morin

Mouillac

et al. 1998

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X-linked nephrogenic diabetes insipidus (NDI) is a rare disease with defective renal and extrarenal arginine vasopressin V2 receptor responses due to mutations in the AVPR2 gene in Xq28. To study the cause of loss of function of mutant V2 receptors, we expressed 12 mutations (N55H, L59P, L83Q, V88M, 497CC-->GG, deltaR202, I209F, 700delC, 908insT, A294P, P322H, P322S) in COS-7 cells. Eleven of these, including P322H, were characterized by a complete loss of function, but the mutation P322S demonstrated a mild clinical and in vitro phenotype. This was characterized by a late diagnosis without any growth or developmental delay and a significant increase in urine osmolality after intravenous 1-deamino[D-Arg8]AVP administration. In vitro, the P322S mutant was able to partially activate the Gs/adenylyl cyclase system in contrast to the other V2R mutants including P322H, which were completely inactive in this regard. This showed not only that Pro 322 is important for proper V2R coupling, but also that the degree of impairment is strongly dependent on the identity of the substituting amino acid. Three-dimensional modeling of the P322H and P322S mutant receptors suggested that the complete loss of function of the P322H receptor could be due, in part, to hydrogen bond formation between the His 322 side chain and the carboxyl group of Asp 85, which does not occur in the P322S receptor.

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Identification of a Single Residue Responsible for Agonist Selectivity in the Oxytocin‐Vasopressin Receptors

Chini

Mouillac

Ala

et al. 1997

Annals of the New York Academy of Sciences

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Y Ala

Tyr115 is the key residue for determining agonist selectivity in the V1a vasopressin receptor.

Properties of a new radioiodinated antagonist for human vasopressin V2 and V1a receptors

Functional studies of twelve mutant V2 vasopressin receptors related to nephrogenic diabetes insipidus

Identification of a Single Residue Responsible for Agonist Selectivity in the Oxytocin‐Vasopressin Receptors

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