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Changes in β-Cell Function in Offspring of Type-2 Diabetic Patients, as per Fasting and Two-Hour Plasma Glucose Levels

机译:每次禁食和两小时血浆葡萄糖水平,2型糖尿病患者后代β细胞功能的变化

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Background The changes in β-cell function in high-risk populations who are apparently in the normal glucose tolerant stage are still under investigation for designing earlier prevention strategies. This study analyzes changes in β-cell function and insulin sensitivity across fasting and two-hour glucose categories spanning normal glucose tolerance (NGT) to impaired glucose tolerance (IGT), in offspring of subjects with type-2 diabetes mellitus (T2DM) compared to the controls without a known family history of T2DM. Methods Offspring of T2DM patients (cases) and individuals without a family history of T2DM (controls) were the subjects for this cross-sectional study. All participants underwent a 75 g oral glucose tolerance test and blood samples were collected for plasma glucose, insulin, C-peptide and proinsulin, at zero, 30, 60, and 120 minutes. Results A total of 358 cases (age 23.0 ± 10.8 years, 54% males) and 287 controls (age 28.4 ± 8.10 years, 65% males) were the subjects of this study. Cases and controls were divided into subgroups based on fasting and two-hour glucose categories spanning NGT to IGT. Compared to the reference category of controls ( 80 mg/dL for fasting glucose and 84 mg/dL for two-hour glucose), cases with IGT had ~60% decline in both β-cell compensation (as measured as disposition index {0-120}) and insulin sensitivity (as measured as whole-body insulin sensitivity index {0-120}); adjusted for age, gender, and body mass index. From lower to higher fasting and two-hour glucose categories, there was a continuous and significant decline in β-cell compensation in both cases and controls. Significant reduction in first-phase insulin secretion, as measured as insulinogenic (0-30) index, was only observed among two-hour glucose categories, not among the fasting glucose categories. In the transition from late NGT cases to IGT cases, there was a significant decline in?β-cell compensation,?first-phase insulin secretion (more prominent than a decline in overall β-cell secretion) and the changes in whole-body insulin sensitivity were not statistically significant. Conclusions The decline in β-cell compensation was continuous and significant in offspring of subjects with type-2 diabetes and controls without a known family history of diabetes from early normal glucose tolerant ranges to impaired glucose tolerant ranges. Compared to the strictest glucose controlled category of controls, approximately 60% decline was observed in β-cell compensation and insulin sensitivity, in impaired glucose tolerant offspring of subjects with type-2 diabetes mellitus.
机译:背景技术在正常葡萄糖耐受阶段显然在正常葡萄糖耐受阶段的高风险群体中的β细胞功能的变化仍在设计前面的预防策略中进行调查。该研究分析了跨越常规葡萄糖耐量(NGT)的禁食和两小时葡萄糖类别,葡萄葡萄素耐受性(IGT)的β细胞功能和胰岛素敏感性的变化在与...相比没有已知的T2DM家族史的控制。方法T2DM患者的后代(病例)和没有T2DM(控制)的家族史的个人是该横断面研究的主题。所有参与者接受了75g口服葡萄糖耐量试验和血样,用于血浆葡萄糖,胰岛素,C-肽和胰岛素,零,30,60和120分钟。结果总共358例(23.0±10.8岁,54%)和287名(28.4±8.10岁,65%的男性)是本研究的主题。基于跨越NGT的禁食和两小时葡萄糖类别,案例和对照分为亚组。与对照的参考分类相比(用于禁食葡萄糖的40mg / dL和两小时葡萄糖的84mg / dl),β-细胞补偿中的IgT含量下降〜60%(按照处置测量指数{0-120})和胰岛素敏感性(以全身胰岛素敏感指数{0-120});调整为年龄,性别和体重指数。从较低到更高的禁食和两小时的葡萄糖类别,两种情况和对照中的β细胞补偿都存在连续而显着下降。在胰岛素原素(0-30)指数中,仅在两小时的葡萄糖类别中观察到一阶段胰岛素分泌的显着降低,而不是空腹葡萄糖类别。在从未晚期患者到IGT病例的过渡中,β-细胞补偿的显着下降,?第一期胰岛素分泌(比整体β细胞分泌的下降更突出)和全身胰岛素的变化敏感性没有统计学意义。结论β-细胞补偿的下降在患有2型糖尿病和对照的受试者的后代是连续的,显着的,没有来自早期正常葡萄糖耐受性的糖尿病的已知家族史,葡萄糖耐受范围受损。与最严格的葡萄糖对照类别相比,β细胞补偿和胰岛素敏感性中观察到大约60%的下降,葡萄糖耐受性患有2型糖尿病患者的血糖耐受性损失。

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