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Does Diabetes Appear in Distinct Phenotypes in Young People? Results of the Diabetes Mellitus Incidence Cohort Registry (DiMelli)

机译:糖尿病在年轻人中表现出明显的表型吗?糖尿病发病队列注册(DiMelli)的结果

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IntroductionThe diabetes mellitus Incidence Cohort Registry (DiMelli) aims to characterize diabetes phenotypes by immunologic, metabolic, and genetic markers. We classified patients into three groups according to islet autoantibody status and examined whether patients with multiple diabetes-associated autoantibodies, one autoantibody, or without autoantibodies differed with respect to clinical, metabolic, and genetic parameters, including an insulin sensitivity (IS) score based on waist, HbA1c, and triglycerides. We also assessed whether metabolic markers predicted the immune status. Materials and MethodsAs of June 2012, 630 patients in Bavaria, Germany, aged 20 years diagnosed with any type of diabetes within the preceding 6 months were registered in DiMelli. We compared the clinical and laboratory parameters between islet autoantibody status defined patient groups. Parameters showing the strongest associations were included in principal component analysis. Receiver operating characteristic curves were used to assess the ability of the IS Score to predict islet autoantibody status. ResultsPatients with multiple islet autoantibodies, one autoantibody, or without autoantibodies were significantly different in terms of BMI percentile, weight loss before diagnosis, fasting C-peptide (all, P0.001), and IS Score (P=0.034). However, principal component analysis revealed no distinct patterns according to autoantibody status. At the optimal IS Score cut-off for predicting islet autoantibody positivity (single compared to none), the specificity was 52.0% and the sensitivity was 86.8%. With respect to prediction of multiple autoantibodies (compared to none), specificity and sensitivity were slightly lower and in combination inferior to those obtained using the BMI percentile and fasting C-peptide. DiscussionThe DiMelli study indicated that patients with and without islet autoantibodies differed with respect to metabolic and genetic markers but there was considerable overlap of phenotypes, and autoantibody status could not be predicted by these parameters. Thus, our results suggest that refined diabetes classification may require both immune and metabolic phenotyping.
机译:简介糖尿病发病队列注册(DiMelli)旨在通过免疫,代谢和遗传标记来表征糖尿病表型。我们根据胰岛自身抗体状况将患者分为三类,并检查具有多种糖尿病相关自身抗体,一种自身抗体或没有自身抗体的患者在临床,代谢和遗传参数(包括基于以下指标的胰岛素敏感性(IS)评分)方面是否存在差异腰,HbA1c和甘油三酸酯。我们还评估了代谢标记物是否可以预测免疫状态。材料和方法截至2012年6月,在德国巴伐利亚州的630名年龄小于20岁的患者在前6个月内被诊断患有任何类型的糖尿病。我们比较了胰岛自身抗体状态定义的患者组之间的临床和实验室参数。主成分分析中包括显示最强关联的参数。接收者操作特征曲线用于评估IS评分预测胰岛自身抗体状态的能力。结果具有多个胰岛自身抗体,一种自身抗体或没有自身抗体的患者在BMI百分率,诊断前体重减轻,空腹C肽(全部,P <0.001)和IS评分(P = 0.034)方面存在显着差异。然而,主成分分析显示根据自身抗体状态没有明显的区别。在用于预测胰岛自身抗体阳性的最佳IS评分临界值(单个与否相比)下,特异性为52.0%,灵敏度为86.8%。关于多种自身抗体的预测(相比之下,没有),特异性和敏感性略低,且组合使用BMI百分位数和空腹C肽获得的特异性和敏感性均逊色。讨论DiMelli研究表明,有和没有胰岛自身抗体的患者在代谢和遗传标记方面有所不同,但表型有相当多的重叠,并且无法通过这些参数预测自身抗体的状态。因此,我们的结果表明,精确的糖尿病分类可能需要免疫和代谢表型。

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