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Arginine 197 of the cholecystokinin-A receptor binding site interacts with the sulfate of the peptide agonist cholecystokinin

Published online by Cambridge University Press:  01 November 1999

VÉRONIQUE GIGOUX
Affiliation:
INSERUM U151, CHU de Rangueil, Bat L3, 31054 Toulouse Cedex, France
BERNARD MAIGRET
Affiliation:
Laboratoire de Chimie Théorique, Université de Nancy, 54506 Vandoeuvre les Nancy, France
CHANTAL ESCRIEUT
Affiliation:
INSERUM U151, CHU de Rangueil, Bat L3, 31054 Toulouse Cedex, France
SANDRINE SILVENTE-POIROT
Affiliation:
INSERUM U151, CHU de Rangueil, Bat L3, 31054 Toulouse Cedex, France
MICHÈLE BOUISSON
Affiliation:
INSERUM U151, CHU de Rangueil, Bat L3, 31054 Toulouse Cedex, France
JEAN-ALAIN FEHRENTZ
Affiliation:
CNRS UMR 5810, Faculté de Pharmacie, 34060 Montpellier, France
LUIS MORODER
Affiliation:
Max Planck Institut für Biochemie, 82143 Martinsried, Germany
DANIELLE GULLY
Affiliation:
Sanofi-Recherche, 195 route d'Espagne, 31036 Toulouse Cedex, France
JEAN MARTINEZ
Affiliation:
CNRS UMR 5810, Faculté de Pharmacie, 34060 Montpellier, France
NICOLE VAYSSE
Affiliation:
INSERUM U151, CHU de Rangueil, Bat L3, 31054 Toulouse Cedex, France
DANIEL FOURMY
Affiliation:
INSERUM U151, CHU de Rangueil, Bat L3, 31054 Toulouse Cedex, France
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Abstract

The knowledge of the binding sites of G protein-coupled cholecystokinin receptors represents important insights that may serve to understand their activation processes and to design or optimize ligands. Our aim was to identify the amino acid of the cholecystokinin-A receptor (CCK-AR) binding site in an interaction with the sulfate of CCK, which is crucial for CCK binding and activity. A three-dimensional model of the [CCK-AR-CCK] complex was built. In this model, Arg197 was the best candidate residue for a ionic interaction with the sulfate of CCK. Arg197 was exchanged for a methionine by site-directed mutagenesis. Wild-type and mutated CCK-AR were transiently expressed in COS-7 cells for pharmacological and functional analysis. The mutated receptor on Arg197 did not bind the agonist radioligand 125I-BH-[Thr, Nle]-CCK-9; however, it bound the nonpeptide antagonist [3H]-SR27,897 as the wild-type receptor. The mutant was ≅1,470- and 3,200-fold less potent than the wild-type CCK-AR to activate G proteins and to induce inositol phosphate production, respectively. This is consistent with the 500-fold lower potency and 800-fold lower affinity of nonsulfated CCK relative to sulfated CCK on the wild-type receptor. These data, together with those showing that the mutated receptor failed to discriminate nonsulfated and sulfated CCK while it retained other pharmacological features of the CCK-AR, strongly support an interaction between Arg197 of the CCK-AR binding site and the sulfate of CCK. In addition, the mutated CCK-AR resembled the low affinity state of the wild-type CCK-AR, suggesting that Arg197–sulfate interaction regulates conformational changes of the CCK-AR that are required for its physiological activation.

Type
Research Article
Information
Protein Science , Volume 8 , Issue 11 , November 1999 , pp. 2347 - 2354
Copyright
© 1999 The Protein Society

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