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The Identifiable Virtual Patient Model: Comparison of Simulation and Clinical Closed-Loop Study Results

机译:可识别的虚拟患者模型:模拟与临床闭环研究结果的比较

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Background: Optimizing a closed-loop insulin delivery algorithm for individuals with type 1 diabetes can be potentially facilitated by a mathematical model of the patient. However, model simulation studies that evaluate changes to the control algorithm need to produce conclusions similar to those that would be obtained from a clinical study evaluating the same modification. We evaluated the ability of a low-order identifiable virtual patient (IVP) model to achieve this goal. Methods: Ten adult subjects (42.5 ± 11.5 years of age; 18.0 ± 13.5 years diabetes; 6.9 ± 0.8% hemoglobin A1c) previously characterized with the IVP model were studied following the procedures independently reported in a pediatric study assessing proportional-integral-derivative control with and without a 50% meal insulin bolus. Peak postprandial glucose levels with and without the meal bolus and use of supplemental carbohydrate to treat hypoglycemia were compared using two-way analysis of variance and chi-square tests, respectively. Results: The meal bolus decreased the peak postprandial glucose levels in both the adult-simulation and pediatric-clinical study (231 ± 38 standard deviation to 205 ± 33 mg/dl and 226 ± 51 to 194 ± 47 mg/dl, respectively; p = .0472). No differences were observed between the peak postprandial levels obtained in the two studies (clinical and simulation study not different, p = .57; interaction p = .83) or in the use of supplemental carbohydrate (3 occurrences in 17 patient days of closed-loop control in the clinical-pediatric study; 7 occurrences over 20 patient days in the adult-simulation study, p = .29). Conclusions: Closed-loop simulations using an IVP model can predict clinical study outcomes in patients studied independently from those used to develop the model.
机译:背景:患者的数学模型可以潜在地促进为1型糖尿病患者优化闭环胰岛素输送算法。但是,评估控制算法更改的模型仿真研究需要得出与从评估相同修改的临床研究中得出的结论相似的结论。我们评估了低阶可识别虚拟患者(IVP)模型实现此目标的能力。方法:按照儿科研究中独立报告的评估比例-积分-微分控制的程序,研究了以IVP模型为特征的十名成年受试者(42.5±11.5岁;糖尿病18.0±13.5岁;血红蛋白A1c 6.9±0.8%)。含或不含50%餐时胰岛素推注。分别使用方差的双向分析和卡方检验,比较了有和无餐时的餐后血糖峰值水平以及使用补充碳水化合物治疗低血糖的情况。结果:在成人模拟和儿科临床研究中,餐后大剂量均降低了餐后血糖峰值(分别为231±38标准偏差至205±33 mg / dl和226±51至194±47 mg / dl; p = .0472)。两项研究(临床和模拟研究无差异,p = .57;相互作用p = .83)或补充碳水化合物的使用(在封闭的17例患者中有3次出现,在儿科临床研究中控制回路;在成人模拟研究中,在20个患者日内发生7次,p = 0.29)。结论:使用IVP模型的闭环模拟可以独立于用于模型开发的患者预测患者的临床研究结果。

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