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首页> 外文期刊>Nature reviews neuroscience >An improved clinical model to predict stimulated C-peptide in children with recent-onset type 1 diabetes
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An improved clinical model to predict stimulated C-peptide in children with recent-onset type 1 diabetes

机译:一种改进的临床模型,以预测近期发病1型糖尿病儿童刺激的C-肽

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Background Stimulated C-peptide measurement after a mixed meal tolerance test (MMTT) is the accepted gold standard for assessing residual beta-cell function in type 1 diabetes (T1D); however, this approach is impractical outside of clinical trials. Objective To develop an improved estimate of residual beta-cell function in children with T1D using commonly measured clinical variables. Subjects/Methods A clinical model to predict 90-minute MMTT stimulated C-peptide in children with recent-onset T1D was developed from the combined AbATE, START, and TIDAL placebo subjects (n = 46) 6 months post-recruitment using multiple linear regression. This model was then validated in a clinical cohort (Hvidoere study group, n = 262). Results A model of estimated C-peptide at 6 months post-diagnosis, which included age, gender, body mass index (BMI), hemoglobin A1c (HbA1c), and insulin dose predicted 90-minute stimulated C-peptide measurements (adjusted R-2 = 0.63, P < 0.0001). The predictive value of insulin dose and HbA1c alone (IDAA1c) for 90-minute stimulated C-peptide was significantly lower (R-2 = 0.37, P < 0.0001). The slopes of linear regression lines of the estimated and stimulated 90-minute C-peptide levels obtained at 6 and 12 months post diagnosis in the Hvidoere clinical cohort were R-2 = 0.36, P < 0.0001 at 6 months and R-2 = 0.37, P < 0.0001 at 12 months. Conclusions A clinical model including age, gender, BMI, HbA1c, and insulin dose predicts stimulated C-peptide levels in children with recent-onset T1D. Estimated C-peptide is an improved surrogate to monitor residual beta-cell function outside clinical trial settings.
机译:背景技术混合膳食耐受试验(MMTT)之后刺激的C肽测量是用于评估1型糖尿病(T1D)的残留β细胞功能的可接受的金标准;然而,这种方法在临床试验之外是不切实际的。目的探讨使用常用临床变量的T1d儿童残留β细胞功能的改进估计。受试者/方法从近期萎缩,开始和潮汐安慰剂(n = 46)6个月使用多元线性回归后,从近期发病T1D预测90分钟MMTT刺激儿童刺激C-肽的临床模型。 。然后在临床队列(HVIDoere研究组,N = 262)中验证该模型。结果诊断后6个月的估计C-肽模型,其中包括年龄,性别,体重指数(BMI),血红蛋白A1C(HBA1C)和胰岛素剂量预测90分钟刺激的C肽测量(调整后的R- 2 = 0.63,P <0.0001)。胰岛素剂量和HBA1C的预测值(IDAA1C)为90分钟刺激的C肽显着降低(R-2 = 0.37,P <0.0001)。估计和刺激的90分钟的线性回归线的斜率在肝脏临床队综合诊断后6和12个月内获得的诊断后均为R-2 = 0.36,P <0.0001,r-2 = 0.37 ,P <0.0001在12个月。结论包括年龄,性别,BMI,HBA1C和胰岛素剂量的临床模型预测有近期发病T1D的儿童刺激的C肽水平。估计的C-肽是一种改善的替代物,用于监测临床试验环境外的残留β细胞功能。

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