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Glycemic variability and glucose complexity in critically ill patients: a retrospective analysis of continuous glucose monitoring data

机译:重症患者的血糖变异性和葡萄糖复杂性:连续血糖监测数据的回顾性分析

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IntroductionGlycemic variability as a marker of endogenous and exogenous factors, and glucose complexity as a marker of endogenous glucose regulation are independent predictors of mortality in critically ill patients. We evaluated the impact of real time continuous glucose monitoring (CGM) on glycemic variability in critically ill patients on intensive insulin therapy (IIT), and investigated glucose complexity - calculated using detrended fluctuation analysis (DFA) - in ICU survivors and non-survivors.MethodsRetrospective analysis were conducted of two prospective, randomized, controlled trials in which 174 critically ill patients either received IIT according to a real-time CGM system (n = 63) or according to an algorithm (n = 111) guided by selective arterial blood glucose measurements with simultaneously blinded CGM for 72 hours. Standard deviation, glucose lability index and mean daily delta glucose as markers of glycemic variability, as well as glucose complexity and mean glucose were calculated.ResultsGlycemic variability measures were comparable between the real time CGM group (n = 63) and the controls (n = 111). Glucose complexity was significantly lower (higher DFA) in ICU non-survivors (n = 36) compared to survivors (n = 138) (DFA: 1.61 (1.46 to 1.68) versus 1.52 (1.44 to 1.58); P = 0.003). Diabetes mellitus was significantly associated with a loss of complexity (diabetic (n = 33) versus non-diabetic patients (n = 141) (DFA: 1.58 (1.48 to 1.65) versus 1.53 (1.44 to 1.59); P = 0.01).ConclusionsIIT guided by real time CGM did not result in significantly reduced glycemic variability. Loss of glucose complexity was significantly associated with mortality and with the presence of diabetes mellitus.
机译:简介血糖变异性是内源性和外源性因子的标志物,而葡萄糖复杂性是内源性葡萄糖调节的标志物,是重症患者死亡率的独立预测因子。我们评估了实时连续葡萄糖监测(CGM)对重症患者接受强化胰岛素治疗(IIT)的血糖变异性的影响,并研究了ICU幸存者和非幸存者的葡萄糖复杂性-使用去趋势波动分析(DFA)计算。方法对两项前瞻性,随机,对照试验进行回顾性分析,其中174例重症患者根据实时CGM系统(n = 63)或根据选择性动脉血糖指导的算法(n = 111)接受了IIT CGM同时盲测72小时。计算标准差,葡萄糖不稳定性指数和平均每日德尔塔血糖作为血糖变异性的指标,并计算葡萄糖复杂性和平均葡萄糖。结果实时CGM组(n = 63)与对照组(n = 111)。与幸存者(n = 138)相比,ICU非幸存者(n = 36)的葡萄糖复杂性显着降低(DFA较高)(DFA:1.61(1.46至1.68)对1.52(1.44至1.58); P = 0.003)。糖尿病与复杂性丧失显着相关(糖尿病(n = 33)与非糖尿病患者(n = 141)(DFA:1.58(1.48至1.65)对1.53(1.44至1.59); P = 0.01)。在实时CGM指导下,血糖变异性并未显着降低;葡萄糖复杂性的丧失与死亡率和糖尿病的存在显着相关。

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