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Endogenous insulin secretion and suppression during and after sepsis in critically ill patients – implications for TGC protocols

机译:重症患者败血症期间和之后的内源性胰岛素分泌和抑制-对TGC方案的影响

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摘要

Introduction:Insulin infusions over 2 U/hr can suppress endogenous insulin secretion in healthy subjects 30-45% [1]. Virtually all tight glycaemic control (TGC) protocols deliver insulin via infusion. This study examines the impact of bolus delivery of insulin in TGC on the endogenous insulin secretion of critically ill patients.Methods:18 patients from the Christchurch Hospital ICU enrolled in a prospective clinical trial studying sepsis each had two sets of blood samples assayed for insulin and C-peptide. The first set was taken at the commencement of the SPRINT TGC protocol for patients with suspected sepsis. The second set was taken when their SIRS score was consistently below 2. Each set had 4 samples taken at: -1, 10, 40 and 60 min following bolus delivery of insulin as required by SPRINT to capture endogenous insulin secretion during the bolus profile. Bolus size was dictated by the protocol, but was in the range 2-6 units. Model-based methods [2] were used to calculate the endogenous insulin secretion rate for each set of samples. The level of suppression was calculated as the ratio of the secretion rate between 5-15 mins (just after peak plasma insulin) and average of the 0-5 min (basal) and 15-60 min (return to basal) secretion rates identified.
机译:简介:超过2 U / hr的胰岛素输注可以抑制健康受试者30-45%的内源性胰岛素分泌[1]。几乎所有严格的血糖控制(TGC)协议都通过输注来输送胰岛素。这项研究探讨了TGC中推注胰岛素对重症患者内源性胰岛素分泌的影响。方法:基督城医院ICU的18名患者参加了一项前瞻性临床研究,研究败血症,每组都有两组血液样本中的胰岛素和C-肽。第一组是在SPRINT TGC方案开始时用于可疑败血症的患者。当第二组的SIRS分数始终低于2时,进行第二组采样。每组在按SPRINT的要求快速输注胰岛素后-1、10、40和60分钟采集4个样品,以在推注过程中捕获内源性胰岛素分泌。规程规定小丸的大小,但范围为2-6个单位。基于模型的方法[2]用于计算每组样品的内源性胰岛素分泌率。抑制水平的计算方法为:5-15分钟(血浆胰岛素峰值之后)的分泌率与0-5分钟(基础)和15-60分钟(恢复基础)的平均分泌率之比。

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