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Nefrología (Madrid)

 ISSN 1989-2284 ISSN 0211-6995

PIETRZAK-NOWACKA, Maria et al. Association of C49620T ABCC8 polymorphism with anthropometric and metabolic parameters in patients with autosomal dominant polycystic kidney disease: a preliminary study. []. , 32, 2, pp.153-159. ISSN 1989-2284.

Background: The aim of the study was to evaluate an association between the C49620T ABCC8 gene polymorphism and anthropometric, biochemical parameters, pancreatic β-cell function and insulin sensitivity among autosomal dominant polycystic kidney disease (ADPKD) patients. Methods: Forty-nine ADPKD patients (M/F: 19/30) and fifty healthy controls (M/F: 22/28) aged above 18 years, with normal kidney function and no diagnosis of diabetes, were enrolled into the study. The ABCC8 (SUR1) C49620T (IVS15-3C/T, rs1799854) genotypes were determined using a PCR-RFLP technique. Results: In the ADPKD group among TT homozygous patients, total body fat content and percentage of fat in body weight were significantly lower than among C allele carriers (16.1±7.7 vs 22.9±7.1kg, p=0.04 and 22.8±6.5 vs 30.0±6.1%, p=0.001, respectively) while total body water was higher (58.4±4.3 vs 53.7±4.0kg, p=0.003). Among TT homozygous controls higher BMI values and LDL-cholesterol levels were observed if compared to C variant carriers (26.3±3.9 vs 23.8±3.4kg/m2 p=0.04 and 133.1±27.0 vs 114.3±35.2mg/dL, p=0.05, respectively), as well as higher area under curve of glucose concentrations (115.9±23.9 vs 102.7± 25.2mmol*h/L, p=0.046) during an oral glucose tolerance test. In the ADPKD group and among controls no association between the investigated polymorphism and secretory function of the pancreatic β cells or insulin sensitivity was found. Conclusion: The C49620T ABCC8 polymorphism is associated with anthropometric risk factors for type 2 diabetes among ADPKD patients, with a protective effect of the TT genotype, but without influence on pancreatic β-cell secretory function or insulin sensitivity.

: ABCC8; ADPKD; Genetic polymorphism; Insulin sensitivity; Obesity; Pancreatic beta-cell secretory function.

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