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首页> 外文期刊>American Journal of Physiology >Simple modeling allows prediction of steady-state glucose disposal rate from early data in hyperinsulinemic glucose clamps
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Simple modeling allows prediction of steady-state glucose disposal rate from early data in hyperinsulinemic glucose clamps

机译:简单的建模允许预测高胰岛素血糖夹具的早期数据的稳态葡萄糖处理率

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After a constant insulin infusion is initiated, determination of steady-state conditions for glucose infusion rates (GIR) typically requires >3 It. The glucose infusion follows a simple time-dependent rise, reaching a plateau at steady state. We hypothesized that nonlinear fitting of abbreviated data sets consisting of only the early portion of the clamp study can provide accurate estimates of steady-state GIR. Data sets from two independent laboratories were used to develop and validate this approach. Accuracy of the predicted steady-state GDR was assessed using regression analysis and Altman-Bland plots, and precision was compared by applying a calibration model. In the development data set (n = 88 glucose clamp studies), fitting the full data set with a simple monoexponential model predicted reference GDR values with good accuracy (difference between the 2 methods —0.37 mg'kg-1 -min-1) and precision [root mean square error (RMSE) = 1.11], validating the modeling procedure. Fitting data from the first 180 or 120 min predicted final GDRs with comparable accuracy but with progressively reduced precision [fitGDR-180 RMSE = 1.27 (.P = NS vs. fitGDR-full); fitGDR-120 RMSE = 1.56 (P < 0.001)]. Similar results were obtained with the validation data set (n = 183 glucose clamp studies), confirming the generalizability of this approach. The modeling approach also derives kinetic parameters that are not available from standard approaches to clamp data analysis. We conclude that fitting a monoexponential curve to abbreviated clamp data produces steady-state GDR values that accurately predict the GDR values obtained from the full data sets, albeit with reduced precision. This approach may help reduce the resources required for undertaking clamp studies
机译:在启动恒定的胰岛素输注后,测定葡萄糖输注速率(GIR)的稳态条件通常需要> 3。葡萄糖输注遵循一个简单的时间依赖上升,达到稳定状态。我们假设仅由钳位研究的早期部分组成的缩写数据集的非线性拟合可以提供对稳态GIR的准确估计。来自两个独立实验室的数据集用于开发和验证这种方法。使用回归分析和Altman-Bland图评估预测稳态GDR的准确性,并且通过施加校准模型进行比较精度。在开发数据集(n = 88葡萄糖钳位研究)中,用简单的单一节目模型拟合完整的数据集,该模型预测参考GDR值,精度良好(2种方法与2种方法之间的差异-0.37 mg'kg-1-min-1)和精度[根均方误差(RMSE)= 1.11],验证建模过程。从前180或120分钟的预测最终GDR拟合数据,具有可比的精度,但逐渐降低精度[FitGDR-180 RMSE = 1.27(.p = ns与fitgdr-full-fife); FITGDR-120 RMSE = 1.56(P <0.001)]。通过验证数据集(n = 183葡萄糖钳位研究)获得了类似的结果,确认了这种方法的普遍性。建模方法还导出从标准方法无法获得钳位数据分析的动力学参数。我们得出结论,将单展曲线拟合到缩写钳位数据产生稳态GDR值,可以精确地预测从完整数据集获得的GDR值,尽管精度降低。这种方法可能有助于减少钳位研究所需的资源

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