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首页> 外文期刊>Journal of Theoretical Biology >Qualitative analysis of subcutaneous Lispro and regular insulin injections for stress hyperglycemia: A pilot numerical study
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Qualitative analysis of subcutaneous Lispro and regular insulin injections for stress hyperglycemia: A pilot numerical study

机译:皮下注射Lispro和常规胰岛素注射治疗应激性高血糖的定性分析:一项初步数值研究

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摘要

Increased glucose variability (GV) is an independent risk factor for mortality in the critically ill; unfortunately, the optimal insulin therapy that minimizes GV is not known. We simulate the glucose-insulin feedback system to study how stress hyperglycemia (SH) states, taken to be a non-uniform group of physiologic disorders with varying insulin resistance (IR) and similar levels of hyperglycemia, respond to the type and dose of subcutaneous (SQ) insulin. Two groups of 100 virtual patients are studied: those receiving and those not receiving continuous enteral feeds. Stress hyperglycemia was facilitated by doubling the gluconeogenesis rate and IR was stepwise varied from a borderline to a high value. Lispro and regular insulin were simulated with dosages that ranged from 0 to 6 units; the resulting GV was analyzed after each insulin injection. The numerical model used consists of a set of non-linear differential equations with two time delays and five adjustable parameters. The results show that regular insulin decreased CV in both patient groups and rarely caused hypoglycemia. With continuous enteral feeds and borderline to mild IR, Lispro showed minimal effect on CV; however, rebound hyperglycemia that increased GV occurred when the IR was moderate to high. Without a nutritional source, Lispro worsened CV through frequent hypoglycemia episodes as the injection dose increased. The inferior performance of Lispro is a result of its rapid absorption profile; half of its duration of action is similar to the glucose ultradian period. Clinical trials are needed to examine whether these numerical results represent the glucose-insulin dynamics that occur in intensive care units, and if such dynamics are present, their clinical effects should be evaluated. (C) 2014 The Authors. Published by Elsevier Ltd.
机译:葡萄糖变异性(GV)增加是重症患者死亡率的独立危险因素;不幸的是,使GV最小化的最佳胰岛素疗法尚不清楚。我们模拟了葡萄糖-胰岛素反馈系统,以研究应激性高血糖(SH)的状态(被认为是具有不同的胰岛素抵抗(IR)和相似的高血糖水平的生理疾病的不均匀组)对皮下类型和剂量的反应(SQ)胰岛素。研究了两组100名虚拟患者:接受和不接受连续肠内饲料的患者。通过使糖异生率加倍来促进应激性高血糖症,IR从临界值逐步升高到高值。用0至6个单位模拟了Lispro和常规胰岛素。每次注射胰岛素后分析所得的GV。所使用的数值模型由一组具有两个时间延迟和五个可调整参数的非线性微分方程组成。结果显示,常规胰岛素在两个患者组中均降低CV,很少引起低血糖症。通过连续的肠内喂养和轻度IR的临界值,Lispro对CV的影响最小。但是,当IR中到高时,会发生GV增加的反弹性高血糖。如果没有营养来源,随着注射剂量的增加,Lispro会因频发的低血糖发作而使CV恶化。 Lispro的不良性能是其快速吸收特性的结果;其作用时间的一半类似于葡萄糖超循环周期。需要进行临床试验以检查这些数值结果是否代表重症监护病房中发生的葡萄糖-胰岛素动力学,如果存在这种动力学,则应评估其临床效果。 (C)2014作者。由Elsevier Ltd.发布

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