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Link between ACE I/D Gene Polymorphism and Dyslipidemia in Diabetic Nephropathy: A Case-control Study from Hyderabad, India

机译:ACE I / D基因多态性与糖尿病肾病多态性和血脂血症之间的联系:印度海德拉巴的病例对照研究

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Introduction: Diabetic nephropathy (DN) is the commonest single cause of end-stage renal failure, and dyslipidemia is a critical risk factor in the occurrence of DN. In the light of recent reports emphasizing the importance of angiotensin I-converting enzyme (ACE) in the modulation of plasma lipids, we sought to evaluate the influence of ACE I/D gene polymorphism with dyslipidemia status among type 2 diabetic (T2D) patients with and without nephropathy in the genetic predisposition and the progression to DN. Method: This study comprised of 600 subjects, which include patients with DN, T2D, and healthy controls (HC). Polymerase chain reaction based genotyping of ACE I/D polymorphism was performed and appropriate statistical analysis was done. Results: Out of the 600 subjects, 20 (10%) of the HC, 73 (36.5%) of the T2D group, and 125 (62.5%) of the DN subjects had dyslipidemia. The D allele (0.62) and DD (42.5) genotype frequencies were higher in the DN group in comparison with T2D and HC ( P 0.05). The genotypes also varied among patients with dyslipidemia (χsup2/sup 5.04; P 0.05) but not in the non-dyslipidemia group. Under the co-dominant model, DD genotype conferred a risk of 1.26 ( P 0.001) toward DN, whereas the ID genotype offered protection from DN among the dyslipidemic subjects (OR = 0.05; P 0.01). In addition, genotype-dependent difference was seen in the plasma lipid levels among study groups. A multiple logistic regression analysis revealed male gender, BMI, HbA1c, TG, HDL, and ACE DD genotype as independent risk factors for the development of DN. Conclusion: The study showed a significant predisposing association of ACE DD genotype with DN and protective effect of ID genotype on DN in the dyslipidemia subgroup.
机译:介绍:糖尿病肾病(DN)是最常见的单一肾功能衰竭原因,血脂血症是DN发生的危险性危险因素。鉴于最近的报道,强调血管紧张素I-转换酶(ACE)在血浆脂质的调节中的重要性,我们试图评估ACE I / D基因多态性对2型糖尿病(T2D)患者的血脂血症状态的影响在遗传易感性中没有肾病和DN的进展。方法:该研究包括600名受试者,包括DN,T2D和健康对照(HC)患者。基于聚合酶链反应的ACE I / D多态性进行了基因分型,并进行了适当的统计分析。结果:出于600个受试者,20%(10%)的HC,73(36.5%)的T2D组,125名(62.5%)的DN受试者具有血脂血症。与T2D和HC相比,DN组中的D等位基因(0.62)和DD(42.5)基因型频率较高(P <0.05)。血脂血症患者的基因型也变化(χ 2 5.04; p <0.05)但不含非血脂血症组。在共拓模型下,DD基因型赋予DN 1.26(P <0.001)的风险,而ID基因型则提供从血脂血症受试者(或= 0.05; P <0.01)中的DN保护。此外,在研究组中的血浆脂质水平中观察到基因型依赖性差异。多逻辑回归分析显示男性性别,BMI,HBA1C,TG,HDL和ACE DD基因型作为DN发展的独立危险因素。结论:该研究表明,在血脂血症亚组中id基因型对DN的DN和ID基因型的保护作用的显着易析出。

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