Interaction between the G1057D variant of IRS-2 and overweight in the pathogenesis of type 2 diabetes

Interaction between the G1057D variant of IRS-2 and overweight in the pathogenesis of type 2 diabetes

The insulin receptor substrate-2 (IRS-2) is a major insulin signalling molecule. IRS-2 inactivation in mice induces a form of diabetes characterized by peripheral insulin resistance and reduced beta cell mass. We tested the hypothesis that a common non-conservative amino acid substitution of IRS-2 (...

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Veröffentlicht in:Human molecular genetics 2000-10, Vol.9 (17), p.2517-2521
Hauptverfasser: MAMMARELLA, Sandra, ROMANO, Ferdinando, DELLA LOGGIA, Fulvio, MARIANI-COSTANTINI, Renato, CAMA, Alessandro, DI VALERIO, Annalisa, CREATI, Beatrice, ESPOSITO, Diana L, PALMIROTTA, Raffaele, CAPANI, Fabio, VITULLO, Paola, VOLPE, Giustino, BATTISTA, Pasquale
Format: Artikel
Sprache:eng
Schlagworte:
Adult
Aged
Alleles
Biological and medical sciences
Blood Glucose - metabolism
Body Mass Index
C-Peptide - blood
Case-Control Studies
Diabetes Mellitus, Type 2 - etiology
Diabetes Mellitus, Type 2 - genetics
Diabetes. Impaired glucose tolerance
Endocrine pancreas. Apud cells (diseases)
Endocrinopathies
Etiopathogenesis. Screening. Investigations. Target tissue resistance
Female
Gene Dosage
Genetic Predisposition to Disease
Genetic Variation
Genotype
Humans
Insulin Receptor Substrate Proteins
insulin receptor substrate-2
Intracellular Signaling Peptides and Proteins
Male
Medical sciences
Middle Aged
Obesity - complications
Odds Ratio
Phosphoproteins - genetics
Polymorphism, Genetic
Regression Analysis
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Zusammenfassung:The insulin receptor substrate-2 (IRS-2) is a major insulin signalling molecule. IRS-2 inactivation in mice induces a form of diabetes characterized by peripheral insulin resistance and reduced beta cell mass. We tested the hypothesis that a common non-conservative amino acid substitution of IRS-2 (G1057D) might interact with overweight in the pathogenesis of type 2 diabetes. The variant was genotyped in 193 Italian patients with type 2 diabetes and 206 control subjects. In the absence of overweight, the risk of type 2 diabetes decreased according to the dosage of the D1057 allele (odds ratio for GD genotype 0.46 [95% CI 0.25-0.86]; DD genotype 0.18 [0.04-0.68]; P for trend = 0.0012). Conversely, the interaction between overweight and genotype increased the risk of type 2 diabetes according to the dosage of the D1057 allele (odds ratio for GD genotype 2.50 [1.11-5.65]; DD genotype 5.74 [1.11-29. 78]; P for trend = 0.0047). Among controls, fasting C-peptide levels, after adjustment for plasma glucose, were inversely related to the dosage of the D1057 allele (P = 0.020). This finding suggested that carriers of the D1057 allele may have higher insulin sensitivity and supported the protective effect of this allele. Conversely, among overweight patients there was a parallel increase in fasting plasma glucose (P for trend = 0.037) and fasting C-peptide according to the dosage of the D1057 allele, suggesting that higher insulin resistance and relative beta cell failure contributed to the increased risk of type 2 diabetes in overweight carriers of this allele. These data provide evidence for a strong association between type 2 diabetes and the G1057D common genetic variant of IRS-2, which appears to be protective against type 2 diabetes in a codominant fashion. Overweight appears to modify the effect of this polymorphism toward a higher risk of type 2 diabetes. Carriers of this polymorphism may represent an elective target for prevention of type 2 diabetes through preventing or treating excessive weight.
ISSN:0964-6906
1460-2083
1460-2083
DOI:10.1093/hmg/9.17.2517