血清Ace和Ace I/D多态性:巴基斯坦2型糖尿病伴和不伴肾病的风险

Hiba Bano, M. Iqbal, Nazish Iqbal Khan, Taseer Ahmed Khan
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摘要

目的:探讨巴基斯坦人群血清血管紧张素转换酶(ACE)水平及ACE I/D多态性与2型糖尿病的关系。方法:随机选取年龄在35 ~ 65岁之间的T2DM确诊患者110例和正常健康对照100例。所有病例均根据随机血糖和空腹血糖水平筛查T2DM,并通过HbA1c检测确诊。采用Salting out法提取外周血基因组DNA,采用插入-缺失多态性对ACE I/D多态性进行基因分型。同时测定血清ACE水平。所有统计分析均采用SPSS 16进行,p值均小于0.05,差异均有统计学意义。Hardy Weinberg平衡(HWE)计算了等位基因频率与预测的任何偏差。采用卡方检验评价ACE多态性与糖尿病风险的相关性。通过二元logistic回归分析,采用优势比和95%置信区间,找出ACE基因分型与糖尿病风险的相关性。结果:分析显示伴有肾病的T2DM患者(平均=158±38.9)和无肾病的T2DM患者(平均= 128.23±46.8)的ACE水平高于对照组(平均= 94.4±28.6)。ACE基因分型与T2DM无显著相关性(÷2 = 7.402, p值=0.116)。而ACE多态基因型DD (O.R= 2.714, 95% CI=0.943 ~ 7.809)组存在糖尿病风险,但结果无统计学意义。然而,女性糖尿病肾病患者没有风险。结论:这些结果表明ACE基因可能与巴基斯坦人群中的2型糖尿病无关。然而,在伴有和不伴有肾病的T2DM患者中,ACE水平较高。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Serum Ace and Ace I/D Polymorphism: Risk of Type 2 Diabetes with and Without Nephropathy in Pakistani Cohort
Objective: To find serum ACE (Angiotensin converting enzyme) level and the role of ACE I/D polymorphism with T2DM (Type 2 Diabetes Mellitus) among the Pakistani cohort. Methods: A total of 110 diagnosed T2DM patients and 100 normotensive healthy controls with an agerange of 35-65 years were randomly selected for this study. All cases were screened for the T2DM based on random and fasting blood sugar levels and confirmed by HbA1c test. Genomic DNA was extracted from peripheral blood samples by the Salting out method and ACE I/D polymorphism was genotyped using insertion-deletion polymorphism. A serum level of ACE was also determined. All statistical analysis was conducted using SPSS 16 and all values are significant at a p-value less than 0.05. Hardy Weinberg Equilibrium (HWE) was calculated for any deviation of allele frequencies from predicted. The Chi-square test was used to evaluate the association between ACE polymorphism and the risk of diabetes. The odds ratio along with a 95% confidence interval via binary logistics regression analysis was used to find out the diabetic risk associated with ACE genotyping. Results: The analysis showed higher ACE levels among T2DM patients with nephropathy (mean =158 ± 38.9) and without nephropathy (mean = 128.23 ± 46.8) as compared to controls (mean = 94.4± 28.6). No significant association (÷2 = 7.402, p-value=0.116) was observed between ACE genotyping and T2DM. However, those who have DD (O.R= 2.714, 95% CI=0.943-7.809) genotype of ACE polymorphism was at risk of diabetes but the results were non-significant. However, no risk was present at the diabetic nephropathy females.Conclusion: These outcomes propose that the ACE gene may not contribute to T2DM in the Pakistanicohort. However, ACE levels were higher among T2DM with and without nephropathy patients.
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