The insulin gene VNTR is associated with fasting insulin levels and development of juvenile obesity.
Document Type
Article
Publication Date
2000
Keywords
Alleles, Body-Mass-Index, Child, Cohort-Studies, Diabetes-Mellitus-Non-Insulin-Dependent, Fasting, Genotype, Human, Insulin, Linear-Models, Minisatellite-Repeats, Obesity, Obesity-Morbid, Polymorphism-Single-Nucleotide, Risk-Factors
First Page
444
Last Page
446
JAX Source
Nat Genet 2000 Dec; 26(4):444-6.
Abstract
In millions of people, obesity leads to type 2 diabetes (T2D; also known as non-insulin-dependent diabetes mellitus). During the early stages of juvenile obesity, the increase of insulin secretion in proportion to accumulated fat balances insulin resistance and protects patients from hyperglycaemia. After several decades, however,beta-cell function deteriorates and T2D develops in approximately 20% of obese patients. In modern societies, obesity has thus become the leading risk factor for T2D (ref. 5). The factors that predispose obese patients to alteration of insulin secretion upon gaining weight remain unknown. To determine which genetic factors predispose obese patients to beta-cell dysfunction, and possibly T2D, we studied single-nucleotide polymorphisms (SNPs) in the region of the insulin gene (INS) among 615 obese children. We found that, in the early phase of obesity, alleles of the INS variable number of tandem repeat (VNTR) locus are associated with different effects of body fatness on insulin secretion. Young obese patients homozygous for class I VNTR alleles secrete more insulin than those with other genotypes.
Recommended Citation
Le SC,
Fallin D,
Schork NJ,
Bougneres P.
The insulin gene VNTR is associated with fasting insulin levels and development of juvenile obesity. Nat Genet 2000 Dec; 26(4):444-6.