Functional and structural characterization of the secretin receptors in rat gastric glands: Desensitization and glycoprotein nature

Author:

Bawab Wafa1,Chastre Eric1,Gespach Christian1

Affiliation:

1. INSERM U55, Hôpital Saint-Antoine, 75571 Paris Cedex 12, France

Abstract

We have documented and characterized the down-regulation of the125I-secretin binding sites and the associated desensitization of the secretin receptor-cAMP system in rat gastric glands. Secretin induced a rapid decrease of the high-affinity125I-secretin binding sites with t1/2=30 min at 37°C. Half-maximal down-regulation and desensitization occurred at 10−9 M secretin, a physiological concentration corresponding to the half-maximal activation of the secretin receptor. The Scatchard parameters of the low-affinity125I-secretin binding sites were unaffected by the pretreatment. This desensitization is heterologous in view of the loss of responsiveness to the truncated glucagon-like peptide 1 (TGLP-1), and pharmacologically selective since the sectetin-related analogue VIP (10−7 M) does not alter the secretin-induced cAMP generation in rat gastric glands. The glycoprotein nature of the secretin receptor has also been demonstrated using WGA-agarose affinity chromatography of the solubilized125I-secretin receptor complex.

Publisher

Portland Press Ltd.

Subject

Cell Biology,Molecular Biology,Biochemistry,Biophysics

Reference32 articles.

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