Genetic Studies of the Sulfonylurea Receptor Gene Locus in NIDDM and in Morbid Obesity Among French Caucasians

Author:

Hani El Habib1,Clément Karine12,Velho Gilberto3,Vionnet Nathalie1,Hager Jörg1,Philippi Anne3,Dina Christian1,Inoue Hiroshi4,Permutt M Alan4,Basdevant Arnaud2,North Michael5,Demenais Florence3,Guy-Grand Bernard2,Froguel Philippe1

Affiliation:

1. CNRS EP 10, Institut Pasteur and C.H.R.U. Lille

2. Départment de Nutrition, Hôtel-Dieu Paris, France

3. INSERM U-358, Hôpital Saint-LouisParis, France

4. Division of Metabolism, Diabetes and Endocrinology, Department of Internal Medicine, Washington University School of Medicine Saint Louis, Missouri

5. Sequana Therapeutics Inc.  La Jolla, California

Abstract

The sulfonylurea receptor (SUR) is a key component in glucose-stimulated insulin secretion. Obesity and NIDDM are frequently associated and share some metabolic abnormalities, suggesting that they might also share some susceptibility genes. Thus, the SUR encoding gene is a plausible candidate for a primary pancreatic β-cell defect and thus for hyperglycemia and weight gain. Through association and linkage studies, we have investigated the potential role of the SUR gene in families with NIDDM and in two independent sets of morbidly obese families. The exon 22 T-allele at codon 761 was more common in patients with NIDDM (7.7%) and morbid obesity (7.8%) than in control subjects (1.8%, P = 0.030 and P = 0.023, respectively). This variant was associated with morbid obesity (odds ratio 3.71, P = 0.017) and NIDDM (odds ratio 2.20, P = 0.04; association dependent on BMI). Although the frequencies for intron 24 variant were similar in all groups, morbidly obese patients homozygous for the c-allele had a more deleterious form of obesity. Sib-pair linkage studies with NIDDM in French Caucasian families gave no evidence for linkage to the SUR locus. However, in one set of the obese families, we found an indication for linkage with a SUR-linked microsatellite marker (D11S419, P = 0.0032). We conclude that in Caucasians, the SUR locus may contribute to the genetic susceptibility to NIDDM and obesity.

Publisher

American Diabetes Association

Subject

Endocrinology, Diabetes and Metabolism,Internal Medicine

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